Drug Development Process Map • Global Drug Trials

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Discovery
Preclinical Development
Phase 1: Clinical Trials
Phase 2 (2a/2b): Clinical Trials
Phase 3: Clinical Trials
Registration
Launch/Post Registration

Decision to enter lead optimization

Lead Chemical Series Selection (LCS)

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Lead chemical series identified. Decision to enter lead optimization Identify unmet user needs, confirm that market requirements & key program assumptions merit advancement to full development.
- DELIVERY
  
  Data sufficient to determine lead candidate. This can be developed from in vitro studies, as well as data from animal models.
- CLINICAL
  
  None, given the early stage of development.
- REGULATORY
  
  None, given the early stage of development.
- COMMONLY ENCOUNTERED DEVELOPMENT RISKS
  
  None, given the early stage of development.
Foundation Investment Decision to Support IND-Enabling Studies

Pre-Clinical Candidate Development

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Lead optimization completed. Decision to develop selected preclinical candidate(s) and enter IND-enabling studies
- DELIVERY
  
  User needs / capabilities / acceptance and market assessments are key inputs into product attributes
  
  • Conduct user assessment of the market opportunity for the new product idea
  
  • Define use case for improving the current standard of care
  
  • Articulate the potential for delivering customer value
  
  • Assess and estimate COGS targets (tied to forecast quantity/volume)
  
  E.g. better clinical outcomes, better economic outcomes, meet / exceed patient adherence, etc.
- CLINICAL
  
  None, given the early stage of development.
- REGULATORY
  
  Regulatory strategy for approval (e.g., geographical filing location, technology type, etc.) guides choice of CMC product design inputs
  
  • Research prior approval packages for similar drug-device combination products
  
  • Consider pricing strategy if product will be covered under national health insurance plans
  
  • Assess intended primary mode of action (FDA) and associated regulatory pathway
  
  • Engage in early and frequent interactions with the NRA in target countries to inform regulatory path and strategy
- COMMONLY ENCOUNTERED DEVELOPMENT RISKS
  
  CMC: Insufficient evaluation of the impact of the chemical characteristics of the Active Pharmaceutical Ingredient (e.g., stability) and its interactions with a device component/excipients/non-API components may result in manufacturing process challenges (e.g., specialized tooling requirements, inability to use commercially available equipment etc.) for design prototypes.
Foundation Investment Decision to Support Phase 1 Trials

First in Human (FIH)

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Initial nonclinical pharmacological, efficacy and safety/toxicity studies and initial drug characterization completed. Initial GMP manufacture process defined. Pre-IND / IND meeting conducted. Decision to enter phase 1 trials
- DELIVERY
  
  Preliminary COGS targets set for the intended use case guide CMC and manufacturing plan
  
  • Conduct user assessment of the market opportunity for the new product idea
  
  • Define use case for improving the current standard of care
  
  • Articulate the potential for delivering customer value
  
  • Develop high level cost-effectiveness, demand forecasts and COGS targets
  
  • Draft package requirements and Instructions For Use (IFU) based on user needs and preliminary prototype
- CLINICAL
  
  Learnings from market assessment and ethnographic studies influence clinical protocols (e.g., understanding device/user needs in clinical settings)
  
  • Incorporate inputs from regulatory interactions into the clinical development plan
  
  • Ensure user (e.g., provider, healthcare workers etc.) training to administer combination product is adequately reflected in clinical protocols
  
  • Evaluate prior combination product development experience as part of site selection and CRO selection process
  
  • Provide estimates of number of products required to support clinical trial
- REGULATORY
  
  For FDA demonstrate compliance with all CGMP regulations (21 CFR 4) applicable to each of the constituent parts included in the combination product
  
  • Engage regulatory experts from Drug, Device, and Combination Product sectors involved in Regulatory planning and interactions with NRA
  
  • Collaborate with NRA to determine further regulatory and clinical requirements for clinical trials and marketing in intended countries
  
  • Incorporate requirements of IND, IDE, and Combination Product regulatory requirements, as guided by the intended market NRA
  
  Plan to handle monitoring and reporting of adverse events and safety issues during clinical trials and post-authorizations.
- COMMONLY ENCOUNTERED DEVELOPMENT RISKS
  
  CMC: Risk management plan (e.g., lack of Quality Systems Regulation) fails to diagnose patient use-related problems until later in the design process, resulting in challenging (and costly) remediation process
  
  Regulatory: Lack of a clear path to approval due to constant evolution of regulatory landscape for certain technology types (e.g., classification as a combination product) may result in product registration delays due to retroactive completion of regulatory requirements
Foundation Investment Decision to Support Phase 2

End of Phase 1 (EP1)

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Phase 1 safety criteria met, feasibility of full scale manufacture and clinical readiness assessed. Decision to enter phase 2 trials
- DELIVERY
  
  Delivery assessments (target market and demand forecast) are inputs to manufacturing scale and COGS estimates
  
  • Conduct market assessments with early prototypes, and develop target market and demand forecasts based on these assessments
  
  • Review user interface requirements in early prototypes
  
  • Draft package requirements and update Instructions For Use (IFU) based on user needs and prototype
- CLINICAL
  
  User capabilities / acceptability verified in the clinical trial influence CMC design risk assessments
  
  • Incorporate inputs from regulatory interactions into the clinical development plan
  
  • Ensure user (e.g., provider, healthcare workers etc.) training to administer combination product is adequately reflected in clinical protocols
  
  • Evaluate prior combination product development experience as part of site selection and CRO selection process
  
  • Provide estimates of number of products required to support clinical trial
- REGULATORY
  
  CMC Risk assessment activities are influenced by regulatory requirements for Design Reviews
  
  • Continue to engage with regulators (as needed)
  
  • Ensure regulatory agency buy-in on Design Verification and Validation Plans
  
  • Update regulatory documents and plans
- COMMONLY ENCOUNTERED DEVELOPMENT RISKS
  
  CMC: Insufficient specifications (e.g., lack of appropriate quality infrastructure, acceptable quality levels, in-process controls or release criteria) may result in product reproducibly failing to meet CQAs
  
  Regulatory: Lack of regulatory agreement on Verification & Validation plan may necessitate additional studies impacting timeline
Foundation Investment Decision to Support Phase 3 Trials

End of Phase 2 (EP2)

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Optimal dose / regimen established, and tech transfer to commercial facility planned or completed. Decision to enter phase 3 trials
- DELIVERY
  
  Updated market assessments and demand forecast informs manufacturing capacity required, Summative Human factors Studies and Instructions for Use are inputs into development of field training materials
  
  • Review product performance with key stakeholders (e.g., procurers, healthcare workers, patients)
  
  • Draft package requirements and update Instructions For Use (IFU) based on user needs and porotype
  
  • Review IFU and test with focus groups (as appropriate)
- CLINICAL
  
  Phase 2 clinical trials offer an opportunity to confirm user experience / preferences assessed in summative human factors study
  
  • Incorporate inputs from regulatory interactions into the clinical development plan
  
  • Ensure user (e.g., provider, healthcare workers etc.) training to administer combination product is adequately reflected in clinical protocols
  
  • Evaluate prior combination product development experience as part of site selection and CRO selection process
  
  • Provide estimates of number of products required to support
- REGULATORY
  
  Regulatory agreement on the acceptability of Design Verification and Validation results triggers capital investments for manufacturing scale up
  
  • Engage with regulators on suitability of results from Design Verification and Validation phase
  
  • Update regulatory documents and plans
  
  Plan to handle monitoring and reporting of adverse events and safety issues during clinical trials and post-authorizations
- COMMONLY ENCOUNTERED DEVELOPMENT RISKS
  
  CMC (Quality)
  
  • Out-of-specification verification and validation results may necessitate costly product re-design and / or process modification
  
  • Lack of definition of design space and plan development may hinder the control of quality critical process parameters and delay process understanding
Foundation Investment Decision to Support Regulatory Dossier Filing

Decision to File (DTF)

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Decision to File: Clinical safety and efficacy demonstrated in phase 3 trials. Decision to file for licensure
- DELIVERY
  
  Plan for market preparation efforts (Launch plan, FAQs, user / provider education etc.) draw on product attributes and IFU (e.g., stability, sterility, use conditions etc.)
  
  • Refine COGS targets to inform commercial scale manufacturing
  
  • Refine cost-effectiveness estimates and pricing expectations in preparation for PQ / launch
  
  • Develop communications / launch strategy regarding clinical trial outcomes, cost-effectiveness relative to existing standard of care etc.
  
  • Draft training / educational materials in preparation for launch
- CLINICAL
  
  Adverse events and complaints outcomes during the clinical trial will inform the post-marketing surveillance and pharmacovigilance strategy
  
  • Support regulatory filing by providing necessary evidence for effectiveness of combination product (based on Phase 3 clinical trial outcome)
  
  • Confirm post-marketing commitments with National Regulatory Agencies in filing geographies
- REGULATORY
  
  Preparation of relevant CMC package, and supporting materials for a pre-filing meeting with the regulatory agency
  
  • Update regulatory documents and plans based on outcomes of pivotal Phase 3 clinical trials
  
  • Prepare regulatory submission documents for commercial product
  
  • Conduct pre-licensure meeting(s) in country of manufacture (as applicable)
- COMMONLY ENCOUNTERED DEVELOPMENT RISKS
  
  CMC (Quality):
  
  • Lack of evidence in reproducibility of product quality during the design transfer process poses regulatory challenges for product filing. For example, as a remediation path, the regulatory agency might require additional bridging studies between pilot and final manufacturing processes
  
  • Lack of updated COGs estimate through refreshed manufacturing strategies and clear plan identifying additional supply sites to be added to the supply network may lead to inadequate supply at affordable prices for excipients, API, disposables and packaging components
Foundation Investment Decision to Support Launch

Prequalification / Local Registration (PQ / LR)

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Prequalification / Local Registration: WHO PQ achieved. Local registration (if required) pursued. Decision to launch
- DELIVERY
  
  Execute on market preparation plan (Launch plan, FAQs, user / provider education etc.) leveraging product attributes and IFU (e.g., stability, sterility, use conditions etc.)
  
  • Execute on launch strategy
  
  • Refine health provider / end user training materials and plan
  
  • Set delivery and country implementation plans, including adequately addressing expectations for post-launch monitoring
- CLINICAL
  
  None, clinical evaluation of the product candidate is complete. Pharmacovigilance addresses potential post-marketing commitments
- REGULATORY
  
  None, regulatory submissions have been completed by this phase of development
- COMMONLY ENCOUNTERED DEVELOPMENT RISKS
  
  Post-marketing commitments, Supply Chain Planning challenges
  
  • Lack of sufficient scale (e.g., PV database infrastructure, staff, Quality and PV Agreements, process and procedures etc.) to meet complaint and adverse events reporting laws and regulations in marketed geographies may hinder the continuous monitoring of product risk
  
  • Insufficient processes for commercial supply S&OP where demand is not understood and continuity of supply is not ensured, may deteriorate relations with suppliers as they are unable to manage the demand on their sites, recover overheads, etc.

Lead Chemical Series Selected
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GOALS/DEFINITIONS: Selection of lead series that meet criteria for progression to Lead Optimization. Drug target validated** and lead identified for optimization. ** It is understood that not all programs will be able to validate the target at this stage in the process
- - Criteria Screening Strategy Established and Target validated (if possible)
  TYPICAL ACTIVITIES
  
  Mechanism of action & target validation (e.g., biomarkers, assays, in vitro / in vivo assessments, etc.)**
  Lead identification strategy defined
  Lead identification screening process (e.g., compound library, HTS, computer-based design, combinatorial chemistry, assays, phenotypic in vitro / in vivo assessments, etc.)
  Selection criteria for ‘actives’
  Screening cascade strategy
  EXAMPLE OF DELIVERABLES FOR REVIEW
  
  Summary of key data to substantiate conclusions
  Illustrative data tables or figures may be reported in an appendix
- - Criteria Lead Identification
  - * CMC experts should be engaged to assess physicochemical properties
  TYPICAL ACTIVITIES
  
  Screening assays (developed and validated)
  Profile hits (e.g., binding affinity, dose-response, specificity, assays, in vitro assessments, etc.)
  Structure-activity relationships
  Assessment of physicochemical properties*
  For phenotypic hits, mechanism of action defined if feasible
  Off-target profiling (e.g., secondary pharmacology, hERG, cytotoxicity, etc.)
  Assessment of reactive metabolite liability
  Drug-drug interaction considerations
  Lead optimization strategy defined
  EXAMPLE OF DELIVERABLES FOR REVIEW
  
  Summary of key data to substantiate conclusions
  Illustrative data tables or figures may be reported in an appendix
Lead Optimization Completed
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GOALS/DEFINITIONS: (1/2) To evaluate basic pharmaceutical properties such as solubility, stability, and physical state of multitude of chemical modifications of the lead scaffold Lead optimization completed and candidate for preclinical candidate development selected (2/2) To evaluate basic pharmaceutical properties such as solubility, stability, and physical state of multitude of chemical modifications of the lead scaffold Initial drug substance characterization completed and preclinical formulation developed
- - (1/2) Criteria Lead candidate optimized
  TYPICAL ACTIVITIES
  
  In vitro, in silico & in vivo (animal) model development and dose response relationships established.
  Preliminary in vitro / in vivo safety / toxicology & in vivo efficacy (e.g., safety pharmacology, acute toxicology, genotoxicity, cytotoxicity, reactive metabolite formation)
  PK and ADME properties optimized and modeling indicates likely to achieve TPP PK goals in human.
  PK-PD relationship established using animal model of disease state (preferred) or alternate functional assay
  Biomarker ID in place for target engagement
  Off-target screening in place and selectivity achieved
  Initial pharmaceutical considerations (e.g. stability, solubility, synthetic feasibility, formulation strategy, etc.)
  Preclinical candidate selection justification package
  EXAMPLE OF DELIVERABLES FOR REVIEW
  
  Summary of key data to substantiate conclusions
  Illustrative data tables or figures may be reported in an appendix
- - (1/2) Criteria Drug combination assessment
  TYPICAL ACTIVITIES
  
  Need for combination considerations
  Assessment strategy
  EXAMPLE OF DELIVERABLES FOR REVIEW
  
  One page summary
- - (1/2) Criteria Candidate molecule meets target product profile
  TYPICAL ACTIVITIES
  
  Alignment with Foundation (intervention) target product profile
  Feasibility and benefit over existing treatments
  EXAMPLE OF DELIVERABLES FOR REVIEW
  
  The cTPP and iTPP may be compared side by side in a table format
  *Candidate progression is discussed at standing grantee update meetings with the investment team
- - (2/2) Criteria Initial drug substance characterization completed
  - * CMC experts should be engaged to assess physicochemical properties
  TYPICAL ACTIVITIES
  
  Molecular & physicochemical properties (e.g., chirality /enantiomer inter-conversion, solubility (pKa, Log P/Log D), permeability (Caco-2 permeability coefficient), BCS classification, etc. )
  Thermal analysis, DS C
  Salt & form screening (e.g., amorphous vs. crystalline, polymorph ID, etc. )
  Drug substance / preliminary drug product stability studies (e.g. solid state drug substance stability, metabolic stability )
  Chemical purity (e.g., impurity identification & profiles, analytical methods )
  Stability studies (e.g., T, pH, humidity, light, metabolic stability, etc.)
  Stable, bioavailable salt/form selected
  EXAMPLE OF DELIVERABLES FOR REVIEW
  
  Summary of key data to substantiate conclusions
  Illustrative data tables or figures may be reported in an appendi x
- - (2/2) Criteria Preclinical formulation to support animal studies completed
  TYPICAL ACTIVITIES
  
  Preliminary drug substance formulation (e.g., salt/form analysis, polymorph characterization, delivery method, confirm bioavailability / PK in animal)
  Formulation considerations related to type of animal studies (e.g. Biomarkers / Preclinical PoC, PKDM and tox studies) and route of administration (e.g. oral / IP / IV / SC)
  Drug substance characterization and formulation for active comparators (known compounds, benchmarks etc.)
  GLP analytical methods for formulation stability and release
  Particle size / oral bioavailability, need for milling / micronization
  EXAMPLE OF DELIVERABLES FOR REVIEW
  
  Summary of key data to substantiate conclusions
  Illustrative data tables or figures may be reported in an appendix
  *Candidate progression is discussed at standing grantee update meetings with the investment team
IND-Enabling Studies Completed
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GOALS/DEFINITIONS: Non clinical safety data and rationale for dose selection. Preclinical drug candidate development activities to support clinical evaluation completed.
- - Criteria Initial nonclinical pharmacological studies completed
  TYPICAL ACTIVITIES
  
  General pharmacology and mechanism(s) of action
  Dose formulation and regimen
  PK, PD, ADME (e.g., biomarker ID, in vitro vs. in vivo assessments, animal model selection, modeling strategies, etc.)
  Off-target screening
  Bioavailability (i.e., tissue, serum, spinal fluid, blood-brain distribution, etc.)
  Development and qualification of supporting bioanalytical and analytical methods (e.g., IR, HPLC, GC, GC/LC MS, etc.) for animal and human application
  EXAMPLE OF DELIVERABLES FOR REVIEW
  
  Pre-IND briefing package, if available; or
  Summary of key data to substantiate conclusions
  Illustrative data tables or figures may be reported in an appendix
- - Criteria Initial nonclinical efficacy studies completed
  TYPICAL ACTIVITIES
  
  Desired outcome measurement criteria
  Demonstration of statistically significant response
  Dose-response relationships & formulation dependency
  Equal or superior efficacy data in comparative studies against licensed and alternative treatments
  Development and qualification of supporting bioanalytical and analytical methods for animal and human application (may overlap with pharmacological characterization)
  EXAMPLE OF DELIVERABLES FOR REVIEW
  
  As above
- - Criteria Initial nonclinical safety / toxicity studies completed
  TYPICAL ACTIVITIES
  
  Acute and subchronic animal toxicology studies, in vitro and in vivo assessments (e.g., genotoxicity screens, dose-response relationships, etc.)
  Establishment of NOAEL, ideally assessing equal or superior safety / toxicity data in comparative studies against licensed and alternative treatments
  Development and qualification of supporting bioanalytical and analytical methods for animal and human application (may overlap with pharmacological characterization)
  EXAMPLE OF DELIVERABLES FOR REVIEW
  
  As above

Candidate Target Product Profile Expectations
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GOALS/DEFINITIONS: Candidate Target Product Profile Agreed. The Candidate Target Product Profile (cTPP) describes the desired attributes of the product and are consistent with mechanism of action and preclinical data.
- - Criteria cTPP developed and agreed
  TYPICAL ACTIVITIES
  
  Drug need, use case, market, and impact on global health
  Product characteristics required to show benefit, such as efficacy, safety, and duration of treatment outlined
  Primary endpoints and secondary endpoints
  Alignment with partner organizations
  EXAMPLE OF DELIVERABLES FOR REVIEW
  
  Use cTPP template – should reflect the desired Intervention TPP (iTPP)
Updated Candidate TPP
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GOALS/DEFINITIONS: Candidate Target Product Profile Agreed. The Candidate Target Product Profile (cTPP) describes the desired attributes of the product and are consistent with mechanism of action and preclinical data.
- - Criteria cTPP further updated to add details
  TYPICAL ACTIVITIES
  
  Drug need, use case, market, and impact on global health
  Product characteristics required to show benefit, such as efficacy, safety, and duration of treatment outlined
  Primary endpoints and secondary endpoints
  Alignment with partner organizations
  Manufacturability
  Route of administration
  Aspirational cost and delivery considerations
  EXAMPLE OF DELIVERABLES FOR REVIEW
  
  Use cTPP template – should reflect the desired Intervention TPP (iTPP)
Updated Candidate TPP
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GOALS/DEFINITIONS: Candidate Target Product Profile Agreed. Identification of commercial partner(s) for launch and full-scale manufacturing of the product.
- - Criteria Updated cTPP with further details
  TYPICAL ACTIVITIES
  
  Indication, use case, and target population
  Global health impact
  Proposed mechanism of action
  Primary endpoints and secondary endpoints
  Manufacturability
  Formulation, dosing, and stability
  Route of administration
  Shelf-life and storage
  Cost and delivery considerations
  Product registration strategy
  EXAMPLE OF DELIVERABLES FOR REVIEW
  
  Use cTPP template – should reflect the desired Intervention TPP (iTPP)
Updated Candidate TPP
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GOALS/DEFINITIONS: Candidate Target Product Profile Agreed. The Candidate Target Product Profile (cTPP) describes the desired attributes of the product and are consistent with mechanism of action and preclinical data.
- - Criteria cTPP developed and agreed
  TYPICAL ACTIVITIES
  
  Indication, use case, and target population
  Global health impact
  Proposed mechanism of action
  Manufacturability
  Formulation, dosing, and stability
  Route of administration
  Shelf-life and storage
  Cost and delivery considerations
  Product registration strategy
  Alignment with partner organizations
  EXAMPLE OF DELIVERABLES FOR REVIEW
  
  Use cTPP template – should reflect the desired Intervention TPP (iTPP)

CMC Development Plan In Place (Drugs)
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GOALS/DEFINITIONS: A detailed plan to complete initial drug substance (DS) and drug product (DP) characterization, and define the initial cGMP manufacturing process. CMC development plan initiated. (The CMC Development Plan is initiated during discovery and preclinical development, and is expected to be in place by the PCD stage gate)
- - Criteria List of activities that will be conducted, that lead to achieving the “Initial DS/DP Characterization” milestone at FIH stage gate
  TYPICAL ACTIVITIES
  
  Complete initial drug product characterization
  Define cGMP manufacturing process
  Complete GMP manufacturing for Ph 1
  Finalize DS characterization & analytical method development
  Manufacture DS at kilo-scale
  Complete DP characterization
  Complete DP package characterization
  Manufacture DP to support the Phase 2 clinical trial
  Manufacturing process optimization
  GMP manufacturing for Ph 3
  Readiness for Tech Transfer
  Technology transfer and validation of raw material, drug substance, and drug product analytical and functional release testing
  Technology transfer and validation of drug substance & drug product manufacturing and packaging processes
  Qualification of commercial-scale facilities
  Commercial launch strategy
  QA/compliance activities
  Ongoing CMC Support to ensure uninterrupted supply of high quality DP in all markets
  EXAMPLE OF DELIVERABLES FOR REVIEW
  
  A detailed plan to achieve the FIH CMC milestones is expected
  Additionally, the Plan should identify potential development risks to PQ, and risk mitigation strategies related to development timeline, costs and resource allocation
  * Items in bold font reflect suggested reporting guidelines for this stage gate
CMC Development Plan Updated (Drugs)
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GOALS/DEFINITIONS: To describe a detailed plan to scale-up manufacturing to provide larger amounts (kilo scale) of clinical trial materials (drug substance and drug product) that will be required for Phase 2 clinical trials. CMC development plan updated.
- - Criteria List of activities that will be conducted, that lead to achieving the “DS/DP Characterized at Kilo-Scale” milestone at EP1 stage gate
  TYPICAL ACTIVITIES
  
  Complete initial drug product characterization
  Define cGMP manufacturing process
  Complete GMP manufacturing for Ph 1
  Finalize DS characterization & analytical method development
  Manufacture DS at kilo-scale
  Complete DP characterization
  Complete DP package characterization
  Manufacture DP to support the Phase 2 clinical trial
  Manufacturing process optimization
  GMP manufacturing for Ph 3
  Readiness for Tech Transfer
  Technology transfer and validation of raw material, drug substance, and drug product analytical and functional release testing
  Technology transfer and validation of drug substance & drug product manufacturing and packaging processes
  Qualification of commercial-scale facilities
  Commercial launch strategy
  QA/compliance activities
  Ongoing CMC Support to ensure uninterrupted supply of high quality DP in all markets
  EXAMPLE OF DELIVERABLES FOR REVIEW
  
  A detailed plan to achieve the EP1 CMC milestones is expected
  Additionally, the Plan should identify potential development risks to PQ, and risk mitigation strategies related to development timeline, costs and resource allocation
CMC Development Plan Updated (Drugs)
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GOALS/DEFINITIONS: To describe a detailed plan to complete process optimization considering feasibility for full-scale manufacturing, including a plan to assess tech transfer readiness to commercial scale manufacturing. cGMP DS manufactured at kilo-scale and scale-up processes defined.
- - Criteria List of activities that will be conducted, that lead to achieving the “Full-Scale DS/DP Manufacturing Process Optimized” and “Tech Transfer and Validation Plan In Place” milestones at EP2 stage gate
  TYPICAL ACTIVITIES
  
  Complete initial drug product characterization
  Define cGMP manufacturing process
  Complete GMP manufacturing for Ph 1
  Finalize DS characterization & analytical method development
  Manufacture DS at kilo-scale
  Complete DP characterization
  Complete DP package characterization
  Manufacture DP to support the Phase 2 clinical trial
  Manufacturing process optimization
  GMP manufacturing for Ph 3
  Readiness for Tech Transfer
  Technology transfer and validation of raw material, drug substance, and drug product analytical and functional release testing
  Technology transfer and validation of drug substance & drug product manufacturing and packaging processes
  Qualification of commercial-scale facilities
  Commercial launch strategy
  QA/compliance activities
  Ongoing CMC Support to ensure uninterrupted supply of high quality DP in all markets
  EXAMPLE OF DELIVERABLES FOR REVIEW
  
  A detailed CMC plan to achieve the EP2 CMC milestones is expected
  Additionally, the Plan should identify potential development risks to PQ, and risk mitigation strategies related to development timeline, costs and resource allocation
  * Items in bold font reflect suggested reporting guidelines for this stage gate
CMC Development Plan Updated (Drugs)
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GOALS/DEFINITIONS: To describe a detailed plan to complete process optimization considering feasibility for full-scale manufacturing, including a plan to assess tech transfer readiness to commercial scale manufacturing. cGMP DS manufactured at kilo-scale and scale-up processes defined.
- - Criteria List of activities that will be conducted, that lead to achieving the “Full-Scale DS/DP Manufacturing Process Optimized” and “Tech Transfer and Validation Plan In Place” milestones at EP2 stage gate
  TYPICAL ACTIVITIES
  
  Complete initial drug product characterization
  Define cGMP manufacturing process
  Complete GMP manufacturing for Ph 1
  Finalize DS characterization & analytical method development
  Manufacture DS at kilo-scale
  Complete DP characterization
  Complete DP package characterization
  Manufacture DP to support the Phase 2 clinical trial
  Manufacturing process optimization
  GMP manufacturing for Ph 3
  Readiness for Tech Transfer
  Technology transfer and validation of raw material, drug substance, and drug product analytical and functional release testing
  Technology transfer and validation of drug substance & drug product manufacturing and packaging processes
  Qualification of commercial-scale facilities
  Commercial launch strategy
  QA/compliance activities
  Ongoing CMC Support to ensure uninterrupted supply of high quality DP in all markets
  EXAMPLE OF DELIVERABLES FOR REVIEW
  
  A detailed CMC plan to achieve the EP2 CMC milestones is expected
  Additionally, the Plan should identify potential development risks to PQ, and risk mitigation strategies related to development timeline, costs and resource allocation
  * Items in bold font reflect suggested reporting guidelines for this stage gate
CMC Development Plan Updated (Drugs)
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GOALS/DEFINITIONS: A detailed plan to address post-launch support – including technical issues during manufacturing and ongoing interactions with regulatory authorities. CMC development plan updated.
- - Criteria List of activities that will be conducted, that lead to achieving the Full-Scale Post-Launch Manufacturing Strategy Updated” milestone at PQ / LR stage gate
  TYPICAL ACTIVITIES
  
  Complete initial drug product characterization
  Define cGMP manufacturing process
  Complete GMP manufacturing for Ph 1
  Finalize DS characterization & analytical method development
  Manufacture DS at kilo-scale
  Complete DP characterization
  Complete DP package characterization
  Manufacture DP to support the Phase 2 clinical trial
  Complete manufacturing process optimization
  Complete GMP manufacturing for Ph 3
  Readiness for Tech Transfer
  Complete technology transfer and validation of raw material, drug substance, and drug product analytical and functional release testing
  Complete technology transfer and validation of drug substance & drug product manufacturing and packaging processes
  Qualification of commercial-scale facilities
  Commercial launch strategy
  QA/compliance activities
  Ongoing CMC Support to ensure uninterrupted supply of high quality DP in all markets
  EXAMPLE OF DELIVERABLES FOR REVIEW
  
  A detailed plan to achieve the PQ / LR CMC milestones is expected
  Additionally, the Plan should identify potential development risks and risk mitigation strategies related to development timeline, costs and resource allocation
  CMC Development Plan should be final at the DTF gate review
  * Items in bold font reflect suggested reporting guidelines for this stage gate

Initial DS/DP Characterization Complete
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GOALS/DEFINITIONS: To evaluate the drug substance (DS) and drug product (DP) that is well-characterized (stable with known impurity profile) and practical to administer in the clinic to ensure ready supply of drug of sufficient quality in Phase 1 clinical trials. Clinical study start-up plan initiated with consideration of feasibility and identification of risks.
- - Criteria Initial drug product characterization completed
  TYPICAL ACTIVITIES
  
  Delivery & formulation strategy to support animal and human studies (e.g., IV, injection, tablet, capsule, oral strip, inhalant, prodrug etc.; assess IP space if special delivery system)
  (For injectables) Consideration for hemolysis studies, adhesion of drug to delivery syringes, tubing, equipment, assess precipitation of drug at injection site (in vitro testing)
  (For prodrug) Characterization in vitro and in vivo conversion to active form
  Particle size considerations and formulation dependency (e.g. milling, micronization, etc.)
  Excipient selection and characterization
  Form-specific physicochemical properties (e.g., bulk & tap densities, flowability, compressibility, pXRD, IR, dissolution, disintegration, etc.)
  Form- and formulation-specific in-use stability studies
  Assess formulation bioavailability / PK for clinical dosing regimen, determine whether “blinding” of clinical formulation needed
  EXAMPLE OF DELIVERABLES FOR REVIEW
  
  Summary of key data to substantiate conclusions
  Illustrative data tables or figures may be reported in an appendix
- - Criteria Initial cGMP manufacturing process defined
  TYPICAL ACTIVITIES
  
  Drug substance manufacturing process overview (e.g., synthetic pathways, intermediate selection, high-level description of unit operations and equipment)
  Drug product manufacturing process overview
  Documentation of external manufacturing plan via Partner Selection Milestone
  Reference standards, analytical GMP methods for drug substance and drug product release and stability, impurities specs for drug substance and drug product
  EXAMPLE OF DELIVERABLES FOR REVIEW
  
  Initial cGMP manufacturing process defined
- - Criteria GMP manufacturing
  TYPICAL ACTIVITIES
  
  GMP DS and Ph1 DP released
  EXAMPLE OF DELIVERABLES FOR REVIEW
  
  Summary of key data e.g. Certificate of Analysis
  *Candidate progression is discussed at standing grantee update meetings with the investment team
DS/DP Characterized at Kilo-Scale
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GOALS/DEFINITIONS: To develop the drug substance (DS) and drug product (DP) to provide larger amounts (kilo scale) of clinical trial materials that will be required for Phase 2 studies. cGMP DS manufactured at kilo-scale and scale-up processes defined.
- - Criteria Drug substance characterization & analytical method development completed/finalized
  TYPICAL ACTIVITIES
  
  Salt & form selection (e.g., amorphous vs. crystalline, polymorph ID, etc.)
  Structural characterization (e.g., enantiomers, diasteriomers, etc.)
  Chemical purity, impurity characterization, and associated analytical methods
  Stability & shelf life studies (e.g., T, pH, humidity, light, etc.)
  Cold chain requirements
  EXAMPLE OF DELIVERABLES FOR REVIEW
  
  Summary of key data to substantiate conclusions
  Illustrative data tables or figures may be reported in an appendix
- - Criteria Drug substance manufactured at kilo-scale
  TYPICAL ACTIVITIES
  
  DS process developed to kilo scale with acceptable yield
  Confirmation of reproducibility of stoichiometry, stable DS physical form and required particle size
  Confirmation of acceptable impurity profile
  EXAMPLE OF DELIVERABLES FOR REVIEW
  
  As above
- - Criteria Drug product characterization & analytical method development completed
  TYPICAL ACTIVITIES
  
  Delivery & formulation strategy (“light touch” quality-by-design [QbD] approach) to support animal and human studies (e.g., IV, injection, tablet, capsule, pediatric dosage form etc.)
  Particle size considerations and formulation dependency
  Excipient selection and characterization
  Chemical purity, impurity characterization, and associated analytical methods
  Form-specific physicochemical properties (e.g., bulk & tap densities, flowability, compressibility, pXRD, IR, dissolution, disintegration, etc.)
  Form- and formulation-specific stability studies
  EXAMPLE OF DELIVERABLES FOR REVIEW
  
  As above
- - Criteria GMP Manufacturing
  TYPICAL ACTIVITIES
  
  Kilo lab GMP DS, Ph 2 DPs Released
  EXAMPLE OF DELIVERABLES FOR REVIEW
  
  Summary of key data, e.g. CoA
  Prior to EP1, CMC will ensure that the DS manufacturing process is developed to produce the required salt, form, and purity profile in larger amounts.
  
  DP formulation components, manufacturing processes and packaging should be final, and scalable so that larger amounts of Phase II clinical study materials can be supplied in a timely manner
  
  *Candidate progression is discussed at standing grantee update meetings with the investment team
Full-scale DS/DP Manufacturing Process Optimized
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GOALS/DEFINITIONS: The development and optimization of the manufacturing process to ensure that the drug substance and product used in the pivotal Phase 3 trial are representative of future commercial product quality. Manufacturing process developed and scaled up.
- - Criteria Manufacturing process optimization completed
  TYPICAL ACTIVITIES
  
  Design-of-experiments and quality-by-design (QbD) methodology with consideration given with ICH Q8, Q9 and Q10 guidance
  Drug substance manufacturing process optimization, scale-up, and pilot studies (e.g., modification of synthetic pathways, intermediate selection, selection of unit operations and equipment, purification process refinement, etc.)
  Drug product manufacturing process optimization, scale-up, and pilot studies (e.g., selection of unit operations to support desired formulation, blending process refinement, etc.)
  Packaging line equipment selection, trials, and optimization
  Process flow diagrams and draft operating parameters
  Operating parameter (yield, purity, and form) relationships
  Waste reduction strategy and product/package end-of-life considerations
  Re-packaging considerations (e.g., end-use packaging vs. packaging for re-distribution)
  EXAMPLE OF DELIVERABLES FOR REVIEW
  
  Summary of key data to substantiate conclusions
  Illustrative data tables or figures may be reported in an appendix
- - Criteria Commercial-scale drug manufacturing feasibility assessment completed
  TYPICAL ACTIVITIES
  
  Evaluation of pilot plant results (product and process) including process economics (e.g. COGs) to make any corrections and a decision on whether or not to proceed with a full-scale plant development
  Safety and ecological assessment of processing and effluents
  EXAMPLE OF DELIVERABLES FOR REVIEW
  
  As above
- - Criteria Drug product package characterization completed
  TYPICAL ACTIVITIES
  
  Leachable/extractable assessment
  Child resistant/senior friendliness testing
  Tamper evidence
  Product compatibility (from package and from environment)
  EXAMPLE OF DELIVERABLES FOR REVIEW
  
  As above
- - Criteria GMP Manufacturing
  TYPICAL ACTIVITIES
  
  GMP Ph 3 DS and DPs released
  EXAMPLE OF DELIVERABLES FOR REVIEW
  
  Summary of key data, e.g. CoA
  * Candidate progression is discussed at standing grantee update meetings with the investment team
  
  ** If a commercial partner has not been identified by EP2, either the PDP will commercialize the products or, PDP will secure adequate funding to conduct future CMC activities
Tech Transfer (DS. Analytical, DP & Packaging), Validation Completed
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GOALS/DEFINITIONS: Completion of launch-related transition of manufacturing processes to full-scale / commercial facilities to ensure uninterrupted supply of high quality product upon regulatory approval. Drug manufacturing process technology transferred and validated.
- - Criteria Technology transfer and validation of raw material, drug substance, and drug product analytical and functional release testing completed
  TYPICAL ACTIVITIES
  
  SOP-driven tech transfer and validation protocols
  Validation package including, at a minimum, the following data for each method used for analytical and functional release testing (in line/at line/off line):
  Specificity
  Sensitivity
  Variability/reproducibility
  EXAMPLE OF DELIVERABLES FOR REVIEW
  
  Summary report
- - Criteria Technology transfer and validation of drug substance & drug product manufacturing and packaging processes completed
  TYPICAL ACTIVITIES
  
  SOP-driven tech transfer and validation protocols
  Overview of manufacturing process, siting, equipment, quality control tools, etc.
  Safety and ecological assessment of drug substance and drug product manufacturing processes
  Validation package including, at a minimum:
  Batch campaign summary
  Final operating conditions
  Control strategy for on-going production
  Three validation batches on stability
  EXAMPLE OF DELIVERABLES FOR REVIEW
  
  Summary report
- - (2/2) Criteria Qualification of commercial-scale facilities completed
  TYPICAL ACTIVITIES
  
  Site master plan (e.g., facility design, maintenance, equipment, calibration schedule, staff training, etc.)
  cGMP certification
  Audits by FDA/NRAs and client
  Commercial-scale batch records
  Change control strategy
  Notice of Event/Deviation reporting mechanism
  Action plan for response to regulatory authority inspections, audits, questions/interactions
  EXAMPLE OF DELIVERABLES FOR REVIEW
  
  Summary report
- - (2/2) Criteria Documentation and Reports
  TYPICAL ACTIVITIES
  
  On-going stability program
  Stability reports
  Process Qualification reports
  Master batch record for commercial manufacturing finalized
  Vendor qualification reports
  SOPs for commercial manufacturing, testing, storage and distribution
  Stability in DS and DP primary containers
  Labeling study report
  Shipping stability study report
  EXAMPLE OF DELIVERABLES FOR REVIEW
  
  Summary report
  *Candidate progression is discussed at standing grantee update meetings with the investment team

Full-Scale Post-Launch Manufacturing Strategy in Place
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GOALS/DEFINITIONS: Development of a strategy to assess operational readiness for full-scale manufacturing launch, including a plan to engage internal CMC experts that have long-term experience with specifics of product and process development with commercial partners. Operational readiness for full-scale manufacturing. (*Full-Scale Post-Launch Manufacturing Strategy is initiated prior to the DTF gate review and is updated & reviewed again at PQ / LR gate review)
- - Criteria Commercial launch strategy
  TYPICAL ACTIVITIES
  
  Product expiry date proposal/strategy for regulatory submission
  Commercial launch strategy for each country market
  Finished product Warehouse qualified and operational
  Shipping validation complete
  EXAMPLE OF DELIVERABLES FOR REVIEW
  
  Summary report
- - Criteria Quality Assurance/Compliance activities
  TYPICAL ACTIVITIES
  
  Product registration
  Facility audit reports
  Audit observation compliance (CAPA, if required)
  Pre-approval inspection strategy, clear roles and responsibilities of partner and CRO/CMO
  EXAMPLE OF DELIVERABLES FOR REVIEW
  
  Summary report
- - Criteria Plan for ongoing CMC Support to ensure uninterrupted supply of high quality DP in all markets
  TYPICAL ACTIVITIES
  
  Establishment of bio-equivalence as appropriate (if the clinical development form and commercial form are not the same)
  Regular meetings with CMOs to monitor supply chain, review of quality incidents
  Ensure corrective actions such as improvements in systems/procedures, staff training
  Ensure timely support of technical support for manufacturing problems
  Evaluate process deviations/excursions during manufacturing that might affect quality
  Scientific evaluation of commercial product stability reports/problems
  Monitor and address changes in raw materials that affect manufacturing/product quality
  Timely submissions of periodic regulatory reports and regulatory agency interactions
  Assess impact of changes in Strategic Demand Forecast, determine whether alternate/additional manufacturing site or additional raw materials suppliers needed
  EXAMPLE OF DELIVERABLES FOR REVIEW
  
  Summary report
  In preparation of DTF stage gate, CMC in the commercial partner organization will complete the activities and reports to demonstrate successful technology transfer and validation, qualification of commercial manufacturing and product release sites, and strategies for commercial launch and future ongoing post-launch commercial production support.
  
  * Candidate progression is discussed at standing grantee update meetings with the investment team
Full-Scale Post-Launch Manufacturing Strategy Updated
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GOALS/DEFINITIONS: An updated strategy to address operational readiness for full-scale manufacturing launch, as more information around identification commercial partners, launch markets and manufacturing scale based on strategic demand forecasts becomes available. Operational readiness for full-scale manufacturing (*Full-Scale Post-Launch Manufacturing Strategy is initiated prior to the DTF gate review and is updated & reviewed again at PQ / LR gate review)
- - Criteria Commercial launch strategy
  TYPICAL ACTIVITIES
  
  Product expiry date proposal/strategy for regulatory submission
  Commercial launch strategy for each country market
  Finished product Warehouse qualified and operational
  Shipping validation complete
  EXAMPLE OF DELIVERABLES FOR REVIEW
  
  Summary report
- - Criteria Quality Assurance/Compliance activities
  TYPICAL ACTIVITIES
  
  Product registration
  Facility audit reports
  Audit observation compliance (CAPA, if required)
  Pre-approval inspection strategy, clear roles and responsibilities of partner and CRO/CMO
  EXAMPLE OF DELIVERABLES FOR REVIEW
  
  Summary report
- - Criteria Plan for ongoing CMC Support to ensure uninterrupted supply of high quality DP in all markets
  TYPICAL ACTIVITIES
  
  Regular meetings with CMOs to monitor supply chain, review of quality incidents
  Ensure corrective actions such as improvements in systems/procedures, staff training
  Ensure timely support of technical support for manufacturing problems
  Evaluate process deviations/excursions during manufacturing that might affect quality
  Scientific evaluation of commercial product stability reports/problems
  Monitor and address changes in raw materials that affect manufacturing/product quality
  Timely submissions of periodic regulatory reports and regulatory agency interactions
  Assess impact of changes in Strategic Demand Forecast, determine whether alternate/additional manufacturing site or additional raw materials suppliers needed
  EXAMPLE OF DELIVERABLES FOR REVIEW
  
  High level plan
  Prior to PQ / LR stage gate, in collaboration with Regulatory, Compliance and other project team members, commercialization partner CMC will prepare a strategy for interactions with regulatory authorities related to regulatory review of registration documents and commercial manufacturing sites. CMC will update, as required, post-launch CMC support strategy
  
  *Candidate progression is discussed at standing grantee update meetings with the investment team

CMC Development Plan in Place (CP/ADDS)
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GOALS/DEFINITIONS: A detailed plan for completing the definition and planning of the combination product at FIH stage gate. CMC development plan updated.
- - Criteria List of activities that will be conducted, that lead to achieving Product Definition and Planning milestone at FIH stage gate
  TYPICAL ACTIVITIES
  
  Plans to complete the following bolded items by the next stage gate:
  User capabilities and preferences assessment
  Ethnographic studies completion
  Hazard identification initiation
  Concept assessment completion
  Design and development plan initiation
  Instructions for Use drafts
  Human Factors Study Plan
  Application risk assessment completion
  Design History File initiation
  Design Input Review completion
  High-level Project Plan and definition of critical product attributes (if prototype available)
  Preliminary device prototype generation
  Design Output Review completion
  Formative human factors study completion
  Design risk assessment completion
  Process risk assessment completion
  Critical component dimensions and specifications definition
  EXAMPLE OF DELIVERABLES FOR REVIEW
  
  Design and Development Plan updates
  Instructions for Use updates
  Design History File updates
  Engineering testing of prototype and conduct simulated use or clinical testing
  Summative human factors study initiated
  Design verification execution
  Design Verification Review completion
  Design validation execution
  Design Validation Review completion
  Design transfer completion
  Design Transfer Review completion
  Supply chain / logistics plan completion
  Complaint handling process definition
  Pharmacovigilance plan completion
  * Completed in PCD Stage
  
  * Items in bold font reflect suggested reporting guidelines for this stage gate
CMC Development Plan in Place Updated (CP/ADDS)
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GOALS/DEFINITIONS: A detailed plan for completing the definition and planning of the combination product at FIH stage gate. CMC development plan updated.
- - (1/2) Criteria List of activities that will be conducted, that lead to achieving Product Definition and Planning milestone at FIH stage gate
  TYPICAL ACTIVITIES
  
  Plans to complete the following bolded items by the next stage gate:
  User capabilities and preferences assessment
  Ethnographic studies completion
  Hazard identification initiation
  Concept assessment completion
  Design and development plan initiation
  Instructions for Use drafts
  Human Factors Study Plan
  Application risk assessment completion
  Design History File initiation
  Design Input Review completion
  High-level Project Plan and definition of critical product Attributes (if prototype available)
  Preliminary device prototype generation
  Design Output Review completion
  Formative human factors study completion
  Design risk assessment completion
  Process risk assessment completion
  Critical component dimensions and specifications definition
  Design and Development Plan updates
  Instructions for Use updates
  Design History File updates
  EXAMPLE OF DELIVERABLES FOR REVIEW
  
  Engineering testing of prototype and conduct simulated use or clinical testing
  Summative human factors study initiated
  Design verification execution
  Design Verification Review completion
  Design validation execution
  Design Validation Review completion
  Design transfer completion
  Design Transfer Review completion
  Supply chain / logistics plan completion
  Complaint handling process definition
  Pharmacovigilance plan completion
  * Items in bold font reflect suggested reporting guidelines for this stage gate
- - (2/2) Criteria Instructions for Use drafted
  TYPICAL ACTIVITIES
  
  Evaluation of appropriate labeling / packaging requirements for the combination product when they are single-entity (e.g., pre-filled syringes, vaginal rings), or physically combined and packaged together (e.g., drug vial with syringe with or without vial adapter) or for separate “cross-labeled” products (e.g., vial adaptor, finger flange with back stop)
  Confirmation that Instructions for Use addresses any use errors or residual user risk related to product safety and efficacy, which cannot be adequately mitigated by product re-design
  EXAMPLE OF DELIVERABLES FOR REVIEW
  
  Summary report containing key data / information or information to substantiate conclusions
  Illustrative data tables or figures may be reported in an appendix
- - (2/2) Criteria Application risk assessment completed
  TYPICAL ACTIVITIES
  
  Identification of potential use problems not apparent from analytical measurements, e.g., the demands associated with use exceed user capabilities
  Initial design review to evaluate adequacy of the design to fulfill intended application
  Appropriate risk mitigation strategies and definition of what residual risk is acceptable
  EXAMPLE OF DELIVERABLES FOR REVIEW
- - (2/2) Criteria High-level Project Plan created and critical product attributes (CPAs) defined (if prototype available)
  TYPICAL ACTIVITIES
  
  Essential processes and equipment required for product development
  Development of prototype tooling and test equipment
  Review of product development plan to understand drug-device interface and alignment between drug stability and device shelf-life attributes. Determine if there are potential interactions between drug and device that would impact the performance/efficacy of the functioning of the device as well as the safety and efficacy of the drug action
  Initiate CMO / suppliers selection process
  EXAMPLE OF DELIVERABLES FOR REVIEW
  
  Summary report containing key data / information or information to substantiate conclusions
  Illustrative data tables or figures may be reported in an appendix
- - (2/2) Criteria Preliminary device prototype generated
  TYPICAL ACTIVITIES
  
  Development of early-stage device prototype for Formative Human Factor Studies
  EXAMPLE OF DELIVERABLES FOR REVIEW
- - (2/2) Criteria Review TPP
  TYPICAL ACTIVITIES
  
  Review TPP developed and determine if modifications are necessary
  EXAMPLE OF DELIVERABLES FOR REVIEW
  * Items in bold font reflect suggested reporting guidelines for this stage gate
CMC Development Plan in Place Updated (CP/ADDS)
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GOALS/DEFINITIONS: A detailed plan for completing design verification and validation of the combination product at EP2 stage gate. CMC development plan updated.
- - (1/2) Criteria List of activities that will be conducted, that lead to achieving Product Definition and Planning milestone at EP2 stage gate
  TYPICAL ACTIVITIES
  
  Plans to complete the following bolded items by the next stage gate:
  User capabilities and preferences assessment
  Ethnographic studies completion
  Hazard identification initiation
  Concept assessment completion
  Design and development plan initiation
  Instructions for Use drafts
  Human Factors Study Plan
  Application risk assessment completion
  Design History File initiation
  Design Input Review completion
  High-level Project Plan and definition of critical product attributes (if prototype available)
  Preliminary device prototype generation
  Design Output Review completion
  Formative human factors study completion
  Design risk assessment completion
  Process risk assessment initiated
  Critical component dimensions and specifications definition
  Design and Development Plan updates
  Instructions for Use updates
  Design History File updates
  EXAMPLE OF DELIVERABLES FOR REVIEW
  
  Engineering testing of prototype and conduct simulated use or clinical testing
  Summative human factors study initiated
  Design verification execution
  Design Verification Review completion
  Design validation execution
  Design Validation Review completion
  Design transfer completion
  Design Transfer Review completion
  Supply chain / logistics plan completion
  Complaint handling process definition
  Pharmacovigilance plan completion
  * Items in bold font reflect suggested reporting guidelines for this stage gate
- - (2/2) Criteria Process risk assessment initiated
  TYPICAL ACTIVITIES
  
  Critical molding and assembly process parameters
  Identification of CMOs and assessment of impact on manufacturing costs and COGS
  Creation of manufacturing flow diagram and assess product demand to verify COGS based on projected demand forecast
  EXAMPLE OF DELIVERABLES FOR REVIEW
  
  Summary report containing key data / information to substantiate conclusions
  Illustrative data tables or figures may be reported in an appendix
- - (2/2) Criteria Critical component dimensions and specifications defined
  TYPICAL ACTIVITIES
  
  Initiation of stability studies development
  Initiation of development packaging and labeling processe
  Transportation studies to determine if there are potential interactions between drug and device during transportation that would impact the performance/efficacy of the functioning of the device as well as the safety and efficacy of the drug actio
  Verification and Validation Plans
  EXAMPLE OF DELIVERABLES FOR REVIEW
- - (2/2) Criteria Instructions for Use updated
  TYPICAL ACTIVITIES
  
  Updated Instructions for Use as data/information becomes available at the appropriate points in the development stage
  EXAMPLE OF DELIVERABLES FOR REVIEW
  
  Summary report containing key data / information to substantiate conclusions
  Illustrative data tables or figures may be reported in an appendix
- - (2/2) Criteria Engineering testing of prototype and conduct simulated use or clinical testing
  TYPICAL ACTIVITIES
  
  Completion of prototype for Summative Human Factors Studies
  EXAMPLE OF DELIVERABLES FOR REVIEW
  * Items in bold font reflect suggested reporting guidelines for this stage gate
CMC Development Plan in Place Updated (CP/ADDS)
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GOALS/DEFINITIONS: A detailed plan for competing design transfer for the combination product at DTF stage gate. CMC development plan updated.
- - (1/2) Criteria List of activities that will be conducted, that lead to achieving Product Definition and Planning milestone at DTF stage gate
  TYPICAL ACTIVITIES
  
  Plans to complete the following bolded items by the next stage gate:
  User capabilities and preferences assessment
  Ethnographic studies completion
  Hazard identification initiation
  Concept assessment completion
  Design and development plan initiation
  Instructions for Use drafts
  Human Factors Study Plan
  Application risk assessment completion
  Design History File initiation
  Design Input Review completion
  High-level Project Plan and definition of critical product attributes (if prototype available)
  Preliminary device prototype generation
  Design Output Review completion
  Formative human factors study completion
  Design risk assessment completion
  Process risk assessment initiated
  Critical component dimensions and specifications definition
  Design and Development Plan updates
  Instructions for Use updates
  Design History File updates
  EXAMPLE OF DELIVERABLES FOR REVIEW
  
  Engineering testing of prototype and conduct simulated use or clinical testing
  Summative human factors study initiated
  Design verification execution
  Design Verification Review completion
  Design validation execution
  Design Validation Review completion
  Design transfer completion
  Design Transfer Review completion
  Supply chain / logistics plan completion
  Complaint handling process definition
  Pharmacovigilance plan completion
  * Items in bold font reflect suggested reporting guidelines for this stage gate
- - (2/2) Criteria Instructions for Use updated
  TYPICAL ACTIVITIES
  
  Updated Instructions for Use as data/information becomes available at the appropriate points in the development stage
  EXAMPLE OF DELIVERABLES FOR REVIEW
  
  Summary report containing key data / information to substantiate conclusions
  Illustrative data tables or figures may be reported in an appendix
- - (2/2) Criteria Process risk assessment completed
  TYPICAL ACTIVITIES
  
  Critical molding and assembly process parameters
  Identification of CMOs and assessment of impact on manufacturing costs and COGS
  Creation of manufacturing flow diagram and assess product demand to verify COGS based on projected demand forecast
  EXAMPLE OF DELIVERABLES FOR REVIEW
- - (2/2) Criteria Review TPP
  TYPICAL ACTIVITIES
  
  Review TPP developed and determine if modifications are necessary
  EXAMPLE OF DELIVERABLES FOR REVIEW
  *Candidate progression is discussed at standing grantee update meetings with the investment team
CMC Development Plan in Place Updated (CP/ADDS)
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GOALS/DEFINITIONS: A detailed plan for completing Post-Launch Surveillance Plan for the combination product at PQ / LR gate. CMC development plan updated.
- - Criteria List of activities that will be conducted, that lead to achieving Product Definition and Planning milestone at PQ / LR stage gate
  TYPICAL ACTIVITIES
  
  Plans to complete the following bolded items by the next stage gate:
  User capabilities and preferences assessment
  Ethnographic studies completion
  Hazard identification initiation
  Concept assessment completion
  Design and development plan initiation
  Instructions for Use drafts
  Human Factors Study Plan
  Application risk assessment completion
  Design History File initiation
  Design Input Review completion
  High-level Project Plan and definition of critical product attributes (if prototype available)
  Preliminary device prototype generation
  Design Output Review completion
  Formative human factors study completion
  Design risk assessment completion
  Process risk assessment initiated
  Critical component dimensions and specifications definition
  Design and Development Plan updates
  Instructions for Use updates
  Design History File updates
  EXAMPLE OF DELIVERABLES FOR REVIEW
  
  Engineering testing of prototype and conduct simulated use or clinical testing
  Summative human factors study initiated
  Design verification execution
  Design Verification Review completion
  Design validation execution
  Design Validation Review completion
  Design transfer completion
  Design Transfer Review completion
  Supply chain / logistics plan completion
  Complaint handling process definition
  Pharmacovigilance plan completion
  * Items in bold font reflect suggested reporting guidelines for this stage gate

Device Design and Development Plan Initiated
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GOALS/DEFINITIONS: Initiate the development of the Design and Development Plan. Establish and maintain plans that: (1) Describe or reference design and development activities (2) Define responsibility for implementation (3) Identify or describe interfaces with different groups or activities (4) Review, document, update and approve plans as design and development evolves.
- - Criteria Design and Development Plan initiated
  TYPICAL ACTIVITIES
  
  Drug-device product Critical Quality Attributes (CQAs) ** and Critical Material Attributes (CMAs), as per the TPP
  Initiation of design control activities including associated documentations
  Initial quality plan
  Technical feasibility assessment
  Alignment on roles and responsibilities for different parties involved (i.e. specification developer, conduct of investigations, IP, publication policy etc.)
  EXAMPLE OF DELIVERABLES FOR REVIEW
Device Design and Development Plan Updated
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GOALS/DEFINITIONS: Update the Design and Development Plan. Establish and maintain plans that: (1) Describe or reference design and development activities (2) Define responsibility for implementation (3) Identify or describe interfaces with different groups or activities (4) Review, document, update and approve plans as design and development evolves.
- - Criteria Design and Development Plan updated
  TYPICAL ACTIVITIES
  
  Updated Design and Development Plan as data / information becomes available at the appropriate points in the development stage
  EXAMPLE OF DELIVERABLES FOR REVIEW
Device Design and Development Plan Updated
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GOALS/DEFINITIONS: Update the Design and Development Plan. Establish and maintain plans that: (1) Describe or reference design and development activities. (2) Define responsibility for implementation. (3) Identify or describe interfaces with different groups or activities . (4) Review, document, update and approve plans as design and development evolves.
- - Criteria Design and Development Plan updated
  TYPICAL ACTIVITIES
  
  Updated Design and Development Plan as data / information becomes available at the appropriate points in the development stage
  EXAMPLE OF DELIVERABLES FOR REVIEW

User Needs and Acceptance
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GOALS/DEFINITIONS: Develop a set of user needs that can be ultimately translated into device requirements. User needs capture what the device does or should do and acceptability of those needs across different geographies.
- Criteria
  
  Intended use, User capabilities and preferences assessed
  Ethnographic studies and user needs conducted
  TYPICAL ACTIVITIES
  
  Assessment of use case, user needs, capabilities, and acceptance (user needs often cannot be finalized before TPP creation) developed within delivery workstream.
  Assessment of market and healthcare ecosystem (procurer requirements (incl. costing considerations), provider, governmental support, etc.) developed within delivery workstream.
  Ethnographic studies to evaluate the care setting, cultural factors, and other factors associated with intended application and setting.
  Task analysis as a precursor to human factors engineering.
Human factors Study Plan Completed
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GOALS/DEFINITIONS: Development of a plan for the conduction of Human Factors studies (Formative and Summative) throughout the program. A study conducted with representative users to assess the adequacy of the combination product user interface design to eliminate or mitigate potential use-related hazards.
- - Criteria Human Factors Study Plan completed
  TYPICAL ACTIVITIES
  
  Intended use statement with benefit of medical device reflected, including consideration on training, education, experience, physical condition, and frequency of use
  User Requirements Specification (URS)
  EXAMPLE OF DELIVERABLES FOR REVIEW
  
  Summary report containing key data / information or information to substantiate conclusions
  Illustrative data tables or figures may be reported in an appendix
Formative Human Factors Study
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GOALS/DEFINITIONS: Conduct Formative Human Factors study and make assessment to modify design as needed. A study conducted on a combination product prototype user interface at one or more stages during the iterative product development process to assess user interaction with the product and identify potential use errors.
- - Criteria Formative Human Factors Study completed
  TYPICAL ACTIVITIES
  
  Results from Human Factors Studies to optimize the device design
  Updated risk assessments based on the results of these studies and develop risk mitigation strategies as needed
  Modified interface design, Instructions for Use, and/or training to address the problems found
  Re‐testing to assess whether mitigation strategies effectively reduced the known risks and did not introduce any new risks
  EXAMPLE OF DELIVERABLES FOR REVIEW
Summative Human Factors Study Completed
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GOALS/DEFINITIONS: Conduct Summative Human Factors Study and compile final results. This test validates that the device, product or system is safe, effective and usable by the all intended user groups. It differs from the formative test in that now you have to use a device that represents exactly the device that is going to be launched to the market.
- - Criteria Summative Human Factors study completed
  TYPICAL ACTIVITIES
  
  Provide evidence of safety and efficacy of the drug-device combination product – from use by representative intended users, under realistic use conditions, for essential and high-risk tasks
  Observe and record errors and/or failures using objective and subjective measures
  Collect user opinion and feedback, particularly related to use problems
  EXAMPLE OF DELIVERABLES FOR REVIEW
Complaint Handling Process Defined
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GOALS/DEFINITIONS: Ensure that product complaints are recorded, processed, and feed into a continuous improvement process for the product. A system to address complaints related to the product. Components of a the system include: process/procedure, trained personnel, and proper record keeping.
- - Criteria Complaint handling process defined
  TYPICAL ACTIVITIES
  
  Establishment of appropriate infrastructure (e.g., a call center, return / replacement process etc.) to handle consumer product complaints
  Definition of procedures to ensure that complaints are processed in a uniform and timely manner
  Root cause analyses for problems reported and feed back into a continuous improvement process to prevent future occurrences
  EXAMPLE OF DELIVERABLES FOR REVIEW

Design History File Initiated
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GOALS/DEFINITIONS: To initiate the compilation of documentation that describes the design history of a finished medical device. The DHF contains or references the records necessary to demonstrate that the design was developed in accordance with the approved design plan.
- - Criteria Design History File initiated
  TYPICAL ACTIVITIES
  
  Design History File to document history of the device design and the design controls elements
  Design Input Requirements
  EXAMPLE OF DELIVERABLES FOR REVIEW
Design History File Updated
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GOALS/DEFINITIONS: To update the compilation of documentation that describes the design history of a finished medical device. The DHF contains or references the records necessary to demonstrate that the design was developed in accordance with the approved design plan.
- - Criteria Design History File updated
  TYPICAL ACTIVITIES
  
  Updated Design History File as data/information becomes available at the appropriate points in the development stage
  Changes made to product need to be captured within the Design History File
  EXAMPLE OF DELIVERABLES FOR REVIEW
Design History File Updated
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GOALS/DEFINITIONS: To update the compilation of documentation that describes the design history of a finished medical device. The DHF contains or references the records necessary to demonstrate that the design was developed in accordance with the approved design plan.
- - Criteria Design History File updated
  TYPICAL ACTIVITIES
  
  Updated Design History File as data/information becomes available at the appropriate points in the development stage
  Changes made to product need to be captured within the Design History File
  EXAMPLE OF DELIVERABLES FOR REVIEW
Design History File Closed
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GOALS/DEFINITIONS: Complete the compilation of documentation that describes the design history of a finished medical device. The DHF contains or references the records necessary to demonstrate that the design was developed in accordance with the approved design plan.
- Criteria
  
  Design History File closed
  TYPICAL ACTIVITIES
  
  Close Design History File when final data/information becomes available
  Changes made to product from CAPA need to be captured within the DHF
Pharmacovigilance Plan in Place
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GOALS/DEFINITIONS: Develop a plan for pharmacovigilance activities. Systems and processes that ensure that information about all suspected adverse reactions that are reported, collected and collated in an accessible manner.
- - Criteria Pharmacovigilance plan in place
  TYPICAL ACTIVITIES
  
  Process to collate and review complaints to determine if they represent reportable adverse drug events
  Process to report adverse events to the appropriate regulatory authority bodies (e.g., for FDA - CDER, CBER, CDRH)
  Develop a strategy to maintain compliance with annual reporting requirements (e.g., Product Safety Update Reports filing for the drug component)
  EXAMPLE OF DELIVERABLES FOR REVIEW

Concepts Screening and Identification
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GOALS/DEFINITIONS: To define and select device concept(s) for drug-device combination product candidate with viable capability to meet the TPP. Concept(s) generated based on based on initial market and user needs and TPP.
- - Criteria Hazard identification initiated
  TYPICAL ACTIVITIES
  
  Use related hazard analysis and assessment, either by application of analytical techniques or by user-based evaluations
  Evaluation of prototype (if prototype is available)
  Potential risk mitigation strategies that may be employed given the product concept and application
  EXAMPLE OF DELIVERABLES FOR REVIEW
  
  Summary of key data / information or information to substantiate conclusions
  Illustrative data tables or figures may be reported in an appendix
- - Criteria Concept assessed
  TYPICAL ACTIVITIES
  
  Evaluation of whether TPP goals can be achieved with an already approved device. If not, definition of the product concept(s) and “proof” that this product, as defined, can be developed and manufactured (based on early testing and existing product data)
  High level assessment of manufacturing capability (changes/new) needed and data suggesting that COGS target can be met
  Anticipated technical risks (high level) and how CMC Development plan for FIH stage gate addresses these risks
  EXAMPLE OF DELIVERABLES FOR REVIEW
  *Candidate progression is discussed at standing grantee update meetings with the investment team
Design Input Review
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GOALS/DEFINITIONS:
Conduct a Design Input Review for the initial requirements that describe the medical device to be produced. Design review is a documented, comprehensive, systematic examination of a design to evaluate the adequacy of the design requirements, to evaluate the capability of the design to meet these requirements, and to identify problems. In general, formal design reviews are intended to:
- provide a systematic assessment of design results, including the device design and the associated designs for manufacturing (DFM) and support processes;
- provide feedback to designers on existing or emerging problems;
- assess project progress; and/or
- provide confirmation that the project is ready to move on to the next stage of development.
- - Criteria Design Input Review conducted
  TYPICAL ACTIVITIES
  
  Conclusions and recommendations from the Design Input Review
  Control plans updated based on risk assessment and Design Input Review
  EXAMPLE OF DELIVERABLES FOR REVIEW
  
  Summary report containing key data / information or information to substantiate conclusions
  Illustrative data tables or figures may be reported in an appendix
Design Output Review
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GOALS/DEFINITIONS:
Conduct a Design Output Review which includes production specifications as well as descriptive materials which define and characterize the design. Design review is a documented, comprehensive, systematic examination of a design to evaluate the adequacy of the design requirements, to evaluate the capability of the design to meet these requirements, and to identify problems. In general, formal design reviews are intended to:
- provide a systematic assessment of design results, including the device design and the associated designs for manufacturing (DFM) production and support processes;
- provide feedback to designers on existing or emerging problems;
- assess project progress; and/or
- provide confirmation that the project is ready to move on to the next stage of development.
- - Criteria Design Output Review conducted
  TYPICAL ACTIVITIES
  
  Conclusions and recommendations from the Design Output Review
  Control plans updated based on risk assessment and Design Output Review
  EXAMPLE OF DELIVERABLES FOR REVIEW
Design Verification and Verification Reviews
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GOALS/DEFINITIONS: To confirm that the design output meets the design input requirements. Objective evidence, in the form of validation testing, to ensure that product design meets specifications, government / industry requirements, and user needs.
- - Criteria Design verification executed
  TYPICAL ACTIVITIES
  
  Execute design verification based on in-process controls and monitoring plan
  Validate analytical tests and methods
  Conduct transportation and stability testing studies
  Initiate documentation of Design Validation Master File, including protocols for Factory Acceptance Tests / Site Acceptance Tests and Installation Qualification / Operational Qualification
  EXAMPLE OF DELIVERABLES FOR REVIEW
  
  Summary report containing key data / information to substantiate conclusions
  Illustrative data tables or figures may be reported in an appendix
- - Criteria Design Verification Review conducted
  TYPICAL ACTIVITIES
  
  Conclusions and recommendations from the Design Verification Review
  Control plans updated based on risk assessment and Design Verification Review
  EXAMPLE OF DELIVERABLES FOR REVIEW
- - Criteria Design validation executed
  TYPICAL ACTIVITIES
  
  Execute design validation based on in-process controls and monitoring plan
  Validate analytical tests and methods
  Conduct transportation and stability testing studies
  Validate molding and assembly process by demonstration of full functionality against design input requirement
  EXAMPLE OF DELIVERABLES FOR REVIEW
- - Criteria Design Validation Review conducted
  TYPICAL ACTIVITIES
  
  Conclusions and recommendations from the Design Validation Review
  Control plans updated based on risk assessment and Design Validation Review
  EXAMPLE OF DELIVERABLES FOR REVIEW
  *Candidate progression is discussed at standing grantee update meetings with the investment team
Design Transfer Review
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GOALS/DEFINITIONS: To ensure device design is translated into product specifications and begin to build-up product inventory for WHO PQ and launch. Formalize procedures that ensure that the device design is correctly translated into product specifications and implement scale-up activities to build-up product inventory, manufactured at commercial scale, in preparation for WHO PQ and launch.
- - Criteria Design transfer completed
  TYPICAL ACTIVITIES
  
  Analytical methods / specifications / acceptance criteria “locked”
  Clear demonstration of specifications that were set / achieved at laboratory scale are applicable at commercial scale
  Confirmation of suppliers being appropriately qualified if the packaging, API + excipients and / or device components will be sourced
  Complete documentation of Design Validation Master File, including protocols for Factory Acceptance Tests / Site Acceptance Tests and Installation Qualification / Operational Qualification
  Updated process risk assessments
  Updated control plans based on risk assessments
  EXAMPLE OF DELIVERABLES FOR REVIEW
  
  Summary report containing key data / information to substantiate conclusions
  Illustrative data tables or figures may be reported in an appendix
- - Criteria Design Transfer Review conducted
  TYPICAL ACTIVITIES
  
  Conclusions and recommendations from the Design Transfer Review
  Control plans updated based on risk assessment and Design Transfer Review
  EXAMPLE OF DELIVERABLES FOR REVIEW
  *Candidate progression is discussed at standing grantee update meetings with the investment team

Design Risk Assessment
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GOALS/DEFINITIONS: Remove a hazard or reduce the level of its risk by adding precautions or control measures, as necessary. Design risk assessment consists of the identification of hazards and the analysis and evaluation of risks associated with device design.
- - Criteria Design risk assessment completed
  TYPICAL ACTIVITIES
  
  Create a risk management report to capture the combination product’s overall residual risk, risk/benefit analysis, and overall conclusion of the product’s safety profile.
  Alignment between design output and user needs defined in user requirements specification (URS)
  Refined device design if Instructions for Use cannot mitigate user errors
  Confirmation that intended use statement is defined
  Definition of critical device attributes
  EXAMPLE OF DELIVERABLES FOR REVIEW
Supply Chain/Logistics Plan in Place
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GOALS/DEFINITIONS: Develop a plan for the supply chain and associated logistics to ensure product can be distributed to the appropriate locations for launch. Turn and move all raw materials to the final combination products and then transfer to customers/users.
- - Criteria Supply chain / logistics plan in place
  TYPICAL ACTIVITIES
  
  Sufficient inventory build up based on demand forecast and management of on-going supply chain
  Transportation design validation reports developed from commercially representative lots
  Verification that incoming, in-process, and final commercial packaging specifications and labeling are in place
  Definition and implementation of tracking capabilities with distributors
  Confirmation of import and export practices meeting local laws and regulations
  Establishment of mechanisms for recalls
  Commercial packs designed and ready for regulatory submission at risk of potential changes by regulators just prior to approval
  EXAMPLE OF DELIVERABLES FOR REVIEW

End of Phase 1 Meeting Scheduled
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GOALS/DEFINITIONS: Gain concurrence with Regulatory Authority on Phase 2 study design. End of Phase 1 Meeting (if needed) with FDA / other NRAs (if applicable) completed (*Specific communication requirements of NRAs should be identified upon initiation of the Regulatory Strategy Plan. If pre-IND meeting (or similar NRA meeting) includes a discussion of Phase 2 plans and there is certainty in the path forward / no protocol adjustments needed based on Phase 1 data / no regulatory requirement, there may not be a need to conduct a formal End of Phase 1 Meeting with NRAs)
- - Criteria Data package necessary for End of Phase 1 meeting completed, endorsed, and submitted to NRA
  TYPICAL ACTIVITIES
  
  Summary of Phase 1 trial results
  Design and scope of Phase 2 study protocol (including study plans, medical monitoring plans, timelines budgets, if required by NRA)
  Proposed clinical development path (e.g. request to use alternate development/authorization pathways (e.g., conditional approval, accelerated, approval, breakthrough designation, orphan designation) and rationale
  Plans for additional nonclinical studies (if any)
  Plans for pediatric studies (including a timeline for protocol finalization, enrollment, completion, and data analysis, or information to support any planned request for waiver or deferral of pediatric studies)
  EXAMPLE OF DELIVERABLES FOR REVIEW
  
  End of Phase 1 briefing package
- - Criteria End of Phase 1 meeting outcomes summarized and development plan modified (if needed)
  TYPICAL ACTIVITIES
  
  Meeting minutes developed by sponsor and also received from NRA (if possible) with documentation on agreements achieved and agreed next steps/actions in End of Phase 1 meeting
  Revised Phase 2 study protocol
  Revised plans for nonclinical studies, pediatric studies, etc.
  EXAMPLE OF DELIVERABLES FOR REVIEW
  
  Regulatory responses to questions
End of Phase 2 Meeting Planned or Scheduled*
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GOALS/DEFINITIONS: Gain concurrence with Regulatory Authority on Phase 3 study design. End of Phase 2 Meeting with NRAs (if applicable) completed. (*Specific communication requirements of NRAs should be identified upon initiation of the Regulatory Strategy Plan)
- - Criteria Data package necessary for End of Phase 2 meeting completed and submitted to NRA
  TYPICAL ACTIVITIES
  
  Summaries of Phase 1/2 trial results
  Design and scope of Phase 3 study protocol (including study plans, medical monitoring plans, timelines and, if required by NRA, budgets)
  Plans for any additional nonclinical studies
  Review/update plans for pediatric studies (including a time line for protocol finalization, enrollment, completion, and data analysis, or information to support any planned request for waiver or deferral of pediatric studies)
  Identification of relevant product issues (i.e., plans to manufacturing scale-up to produce product for commercial scale and the need for comparability testing relative to the product used in Phase 1/2 clinical studies)
  Planned label, especially highlighting desired wording for indications (s) and any safety claims desired to make
  If a Special Protocol Assessment agreement is desired (US specific), also requires:
  Detailed protocol design (i.e., proposed size, power calculation, choice of study endpoints, choice of control, duration, methods of assessment)
  Data analysis plan
  Role of the study in the overall development plan
  EXAMPLE OF DELIVERABLES FOR REVIEW
  
  End of Phase 2 briefing package
- - Criteria End of Phase 2 meeting outcomes summarized and development plan modified (if needed)
  TYPICAL ACTIVITIES
  
  Meeting minutes prepared by sponsor and shared with NRA; get NRA minutes (if possible). Document agreements achieved and next steps/actions agreed at end of Phase 2 meeting
  Revised Phase 3 study protocol
  Revised plans for nonclinical studies or pediatric studies
  EXAMPLE OF DELIVERABLES FOR REVIEW
  
  Regulatory responses to questions
Pre-licensure Meeting Scheduled*
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GOALS/DEFINITIONS: Gain concurrence with Regulatory Authority on licensure. Pre-licensure meeting(s) in country of manufacture conducted. (*Specific communication requirements of National Regulatory Authorities (NRA) should be identified upon initiation of the Regulatory Strategy Plan)
- - Criteria Requirements for pre-licensure meeting(s) in country of manufacture completed; endorsed, submitted to NRA(s)
  TYPICAL ACTIVITIES
  
  Safety and efficacy data from all clinical trials
  Product release specifications (including pre-approval inspection of manufacturing facilities)
  Stability data to support expiration dating
  Claims and indication statement in the product label
  If applicable, agreement on deferral (or waiver) of pediatric studies
  Plans for any post-approval clinical studies and pharmacovigilance plan
  Information on transition from clinical to commercial-scale manufacture (i.e., establishing comparability of the Phase 3 and commercial products)
  Plans for organizing the content of the application and the submission type (paper vs. electronic)
  Determine if any type of advisory committee meeting will be necessary (if applicable)
  Determine schedule/route of communications with NRA during review process
  EXAMPLE OF DELIVERABLES FOR REVIEW
  
  End of Pre-licensure briefing package
- - Criteria Post-meeting debrief and development strategy adjustment (if required) completed
  TYPICAL ACTIVITIES
  
  Minutes of meeting prepared by sponsor. NRA minutes obtained (if possible). Review of decisions and recommendations made at the meeting.
  Action plan to address highlighted development issues (if any) prior to filing of application
  EXAMPLE OF DELIVERABLES FOR REVIEW
  
  Regulatory responses to questions
WHO PQ or First Local Registration
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GOALS/DEFINITIONS: WHO PQ dossier submission. WHO PQ meeting data submission, and/or meeting decision and recommendations for product prequalification. (Note: PQ meeting with QSS conducted at the end of phase 2)
- - Criteria Safety and efficacy demonstrated
  TYPICAL ACTIVITIES
  
  Safety and efficacy data from all clinical trials
  Product release specifications (including pre-approval inspection of manufacturing facilities)
  Stability data to support expiration dating (e.g., cold chain requirements/suitability for use under field conditions, shelf life and remaining shelf life at time of shipment)
  EXAMPLE OF DELIVERABLES FOR REVIEW
  
  Notification of submission date
- - Criteria Relevance to target population demonstrated
  TYPICAL ACTIVITIES
  
  Relevance of the available clinical data to the UN target population
  Specific requirements of UN procurers
  Any specific advisory group recommendations needed/documented/addressed
  EXAMPLE OF DELIVERABLES FOR REVIEW
  
  Summary of special requirements met
- - Criteria WHO tender specifications met
  TYPICAL ACTIVITIES
  
  Packaging: Volume of cold space required (if any), primary and secondary packaging characteristics
  Suitability of presentation (e.g., tablets, vials, ampoules or prefilled auto-dispensable syringes)
  Applicability packaging requirements
  Adequacy of information on labels for package: all relevant information is stated, insert reflects product characteristics and does not contradict model inserts and WHO policies; availability in all required languages
  Tertiary packaging prepared according to the WHO shipping guidelines and are properly validated
  EXAMPLE OF DELIVERABLES FOR REVIEW
  
  Summary of product suitability requirements met
- - Criteria Pharmacovigilance (PV) Plan
  TYPICAL ACTIVITIES
  
  Particularly relevant if the drug is intended for launch only in low income countries where passive PV is insufficient. Plan can include:
  Summary of key identified and potential risks
  Action Plan for collecting reports of adverse reaction, active monitoring, evaluating and reporting of safety issues to regulatory authorities (e.g., Periodic Safety Update Reports, ADRs: Adverse Drug Reactions)
  Overall PV plan for the product bringing together the actions for all individual safety issues
  EXAMPLE OF DELIVERABLES FOR REVIEW
  
  High level plan

Pre-IND Meeting Scheduled* (Optional)
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GOALS/DEFINITIONS: Gain concurrence with Regulatory Authority on Phase 1 study design. Data package necessary for pre-IND and/or IND meeting (or NRA equivalent meeting) submission, and/or meeting opinion. (*Specific communication requirements of National Regulatory Authorities (NRAs) should be identified upon initiation of the Regulatory Strategy Plan)
- - Criteria Package for pre-IND meeting submission (NRA equivalent meeting) prepared
  - Ethics committee review process understood and interplay with pre-IND meeting understood
  TYPICAL ACTIVITIES
  
  List of specific questions and input sought from regulatory agency
  Summary of drug characterization data (e.g., basic molecular properties, physicochemical properties, purity, stability, preliminary formulation concept, etc.)
  Summary of initial nonclinical assessments
  PK, PD, ADME
  Efficacy and activity
  Safety
  Manufacture plan & initial specs developed as required for clinical trial supplies
  Outline of follow-on nonclinical studies
  Outline of clinical plan (which may leverage Clinical Development Plan and Clinical Readiness milestones content), including:
  Rationale for intended use
  Studies supporting dosing and duration
  Appropriateness of safety monitoring techniques
  Assurance of clinical trial supply quality
  Phase 1 trial design & protocol
  Inclusion / exclusion criteria; safety monitoring procedures
  High-level plans for Phase 2 study
  EXAMPLE OF DELIVERABLES FOR REVIEW
  
  Pre-IND briefing package
- - Criteria Post-meeting debrief and development strategy adjustment (if required) completed
  TYPICAL ACTIVITIES
  
  Review of decisions and recommendations made at the meeting
  Action plan to address highlighted development issues (if any) prior to filing of clinical trials application
  EXAMPLE OF DELIVERABLES FOR REVIEW
  
  Regulatory responses to questions
IND Submitted to Regulatory Agency
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GOALS/DEFINITIONS: Gain concurrence with Regulatory Authority on Phase 1 study design. Track the regulatory approval to enter to Phase 1 studies. (*Specific communication requirements of National Regulatory Authorities (NRAs) should be identified in upon initiation of the Regulatory Strategy Plan)
- - Criteria IND application package (or similar NRA clinical trials package) prepared, endorsed, submitted, and received by regulatory agency
  TYPICAL ACTIVITIES
  
  List of regulatory agency requirements (for example)
  Drug substance & drug product properties
  Stability data
  Relevant animal PK and disease model data
  Argument for acceptability of preclinical candidate safety profile
  Demonstrated in vitro and/or in vivo efficacy/activity, as applicable
  Argument for acceptability of drug interaction profile
  Feasibility of cGMP manufacture & CMC information relevant to clinical trial supplies
  Previous human exposure (if available)
  Argument for acceptability of clinical dosage form
  Clinical proof of concept plan
  Proposed clinical trial protocols
  Application package aligned with agency requirements
  Confirmation of application receipt by FDA / NRA
  EXAMPLE OF DELIVERABLES FOR REVIEW
  
  Notification of submission date
- - Criteria US IND application response (if any) or similar NRA application approved
  TYPICAL ACTIVITIES
  
  If filed with US FDA, confirmation that no response from the US FDA was received within 30 days after the agency’s receipt of the IND application
  No response confirmation and/or approval confirmation from other NRAs as required for their clinical trials applications
  Ethics Committee action
  EXAMPLE OF DELIVERABLES FOR REVIEW
  
  Notification of Regulatory Authority response (if any) and any impact to timeline or study design

Regulatory Strategy and Plan in Place
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GOALS/DEFINITIONS: Regulatory path and plan in place. Plan for proposed regulatory path through life-cycle of the product. (* An iterative document that is initiated at FIH, updated continually along the development process, and reviewed through to DTF)
- - Criteria Proposed regulatory path through life-cycle of product defined, including:
  - Clinical development
    Licensure
    WHO PQ (if needed)
    Post-authorization safety surveillance and further product development
    Include any specific plans to use alternative development pathways (conditional, accelerated, breakthrough) or registration processes (article 58, tropical voucher, orphan)
  TYPICAL ACTIVITIES
  
  Prioritized list of countries where the drug is intended to be introduced¹
  Understanding of country-specific regulatory requirements
  Type of submissions (original, supplement/variation, line extension, etc)
  Significant/unique requirements²
  Required HA communications and timing
  Plans for NRA engagement during development to gain feedback and agreement with development and filing strategy
  Key regulatory risks and risk mitigation plans
  Plan to ensure proposed indication and labeling aligns with TPP and donor/utilization requirements
  Plan for approval and protocol review for clinical trial starts in target countries
  Plan to handle monitoring and reporting of adverse events and safety issues during clinical trials and post-authorizations
  WHO PQ applicability/programmatic suitability, plan to pursue WHO PQ (if applicable)
  Plans for WHO PQ engagement by end of phase 2 (if applicable)
  EXAMPLE OF DELIVERABLES FOR REVIEW
  
  Updated throughout life-cycle of product reflecting new data and priorities as they develop
  Required at each gate: Detailed plan with timeline and resources for the next phase of development (e.g. detailed plan for Phase 1 required at the FIH gate review), and high-level / draft plan focusing on risk identification and mitigation for all subsequent phases of development
  Items in bold font reflect suggested reporting guidelines for this stage gate
  
  1 If India and China are among the likely target countries, content is required at FIH. Otherwise it applies at EP2.
  
  2 Specific requirements associated with Chinese Pharmacopeia should be updated early
Regulatory Strategy and Plan Updated
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GOALS/DEFINITIONS: Regulatory path and plan in place. Plan for proposed regulatory path through life-cycle of the product. (*An iterative document that is initiated at FIH, updated continually along the development process, and reviewed through to DTF)
- - Criteria Proposed regulatory path through life-cycle of product defined, including clinical development, licensure, WHO PQ (if needed), and post-authorization safety surveillance and further product development
  - Include any specific plans to use alternative development pathways (conditional, accelerated, breakthrough) or registration processes (article 58, tropical voucher, orphan)
  TYPICAL ACTIVITIES
  
  Prioritized list of countries where the drug is intended to be introduced¹
  Understanding of country-specific regulatory requirements
  Type of submissions (original, supplement/variation, line extension, etc)
  Significant / unique requirements²
  Required HA communications and timing
  Plans for NRA engagement during development to gain feedback and agreement with development and filing strategy
  Key regulatory risks and risk mitigation plans
  Plan to ensure proposed indication and labeling aligns with TPP and donor/utilization requirements
  Plan for approval and protocol review for clinical trial starts in target countries
  Plan to handle monitoring and reporting of adverse events and safety issues during clinical trials and post-authorizations
  WHO PQ applicability/programmatic suitability, plan to pursue WHO PQ (if applicable)
  Plans for WHO PQ engagement by end of phase 2 (if applicable)
  EXAMPLE OF DELIVERABLES FOR REVIEW
  
  Updated throughout life-cycle of product reflecting new data and priorities as they develop
  Required at each gate: Detailed plan with timeline and resources for the next phase of development (e.g. detailed plan for Phase 1 required at the FIH gate review), and high-level / draft plan focusing on risk identification and mitigation for all subsequent phases of development
  Items in bold font reflect suggested reporting guidelines for this stage gate
  
  1 If India and China are among the likely target countries, content is required at FIH. Otherwise it applies at EP2.
  
  2 Specific requirements associated with Chinese Pharmacopeia should be updated early
Regulatory Strategy and Plan Updated
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GOALS/DEFINITIONS: Regulatory path and plan in place. Plan for proposed regulatory path through life-cycle of the product. (*An iterative document that is initiated at FIH, updated continually along the development process, and reviewed through to DTF).
- - Criteria Proposed regulatory path through life-cycle of product defined, including clinical development, licensure, WHO PQ (if needed), and post-authorization safety surveillance and further product development
  - Include any specific plans to use alternative development pathways (conditional, accelerated, breakthrough) or registration processes (article 58, tropical voucher, orphan)
  TYPICAL ACTIVITIES
  
  Prioritized list of countries where the drug is intended to be introduced
  Understanding of country-specific regulatory requirements
  Type of submissions (original, supplement/variation, line extension, etc.)
  Significant/unique requirements
  Required HA communications and timing
  Plans for NRA engagement during development to gain feedback and agreement with development and filing strategy
  Key regulatory risks and risk mitigation plans
  Plan to ensure proposed indication and labeling aligns with TPP and donor/utilization requirements
  Plan for approval and protocol review for clinical trial starts in target countries
  Plan to handle monitoring and reporting of adverse events and safety issues during clinical trials and post-authorizations
  WHO PQ applicability/programmatic suitability, plan to pursue WHO PQ (if applicable)
  Plans for WHO PQ engagement by end of phase 2 (if applicable)
  EXAMPLE OF DELIVERABLES FOR REVIEW
  
  Updated throughout life-cycle of product reflecting new data and priorities as they develop
  Required at each gate: Detailed plan with timeline and resources for the next phase of development (e.g. detailed plan for Phase 1 required at the FIH gate review), and high-level / draft plan focusing on risk identification and mitigation for all subsequent phases of development
  *Items in bold font reflect suggested reporting guidelines for this stage gate
Regulatory Strategy and Plan Updated
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GOALS/DEFINITIONS: Regulatory path and plan in place. Plan for proposed regulatory path through life-cycle of the product. (Regulatory Strategy Plan is initiated prior to the FIH gate review and is updated & reviewed during development through to the DTF gate review).
- - Criteria Proposed regulatory path through life-cycle of product defined, including clinical development, licensure, WHO PQ (if needed), and post-authorization safety surveillance and further product development
  - Include any specific plans to use alternative development pathways (conditional, accelerated, breakthrough) or registration processes (article 58, tropical voucher, orphan)
  TYPICAL ACTIVITIES
  
  Prioritized list of countries where the drug is intended to be introduced
  Understanding of country-specific regulatory requirements
  Type of submissions (original, supplement/variation, line extension, etc.)
  Significant/unique requirements
  Required HA communications and timing
  Plans for NRA engagement during development to gain feedback and agreement with development and filing strategy
  Key regulatory risks and risk mitigation plans
  Plan to ensure proposed indication and labeling aligns with TPP and donor/utilization requirements
  Plan for approval and protocol review for clinical trial starts in target countries
  Plan to handle monitoring and reporting of adverse events and safety issues during clinical trials and post-authorizations
  WHO PQ applicability/programmatic suitability, plan to pursue WHO PQ (if applicable)
  Plans for WHO PQ engagement by end of phase 2 (if applicable)
  EXAMPLE OF DELIVERABLES FOR REVIEW
  
  Updated throughout life-cycle of product reflecting new data and priorities as they develop
  Required at each gate: Detailed plan with timeline and resources for the next phase of development, and high-level/draft plan focusing on risk identification and mitigation for all subsequent phases of development
  *Items in bold font reflect suggested reporting guidelines for this stage gate

Study Start-up Activities Initiated
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GOALS/DEFINITIONS: Start-up activities are initiated to enable timely Phase 2 start Clinical study start-up plan initiated with consideration of feasibility and identification of risks
- - Criteria Clinical trial designed
  TYPICAL ACTIVITIES
  
  Protocol design and scope for Phase 1 (including study plans, medical monitoring plans, timelines and budgets) to support both NRA approval and WHO PQ
  An overview of the clinical development path (i.e., request for conditional approval) and rationales
  Updates to Investigator’s Brochure for the next phase of development. (e.g., prior to First in Human include Core Safety Information from toxicology study)
  EXAMPLE OF DELIVERABLES FOR REVIEW
  
  Protocol synopsis
  Investigator Brochure
- - Criteria Clinical trial site feasibility completed
  TYPICAL ACTIVITIES
  
  Plan for site assessment (may include audit) including considerations such as infrastructure, capability, supply chain feasibility, capacity, etc.
  Understanding of required approval process to conduct clinical studies at all potential study sites and identifying risks
  EXAMPLE OF DELIVERABLES FOR REVIEW
  
  Summary report
- - Criteria Clinical vendors/ CRO identified and site initiation activities conducted
  TYPICAL ACTIVITIES
  
  Scope of work required (e.g., site selection, site initiation, data management, process & method development, etc.) and agreed metrics to monitor trial progress
  Partner engagement strategy (e.g., outsourced activity, insourced activity, consultation, etc.)
  Examples of past vaccine trial experience in the disease area/geographic area
  Understanding of the stepwise clinical trial approval process, engaging with local regulatory authorities, ethics committee etc.
  Existing network of investigators and study sites
  Audit record of clinical study sites and track record of staff GCP training
  Completion of site initiation activities
  EXAMPLE OF DELIVERABLES FOR REVIEW
  
  Summary report
- - Criteria Clinical assay readiness
  TYPICAL ACTIVITIES
  
  Relevant clinical assays need to be available prior to entering clinical studies
  EXAMPLE OF DELIVERABLES FOR REVIEW
  
  Summary of assay qualification
Study Start-up Activities Initiated
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GOALS/DEFINITIONS: Start-up activities are initiated to enable timely Phase 1 start Clinical study start-up plan initiated with consideration of feasibility and identification of risks
- - Criteria Clinical trial designed
  TYPICAL ACTIVITIES
  
  Protocol design and scope for Phase 1 (including study plans, medical monitoring plans, timelines and budgets) to support both NRA approval and WHO PQ
  An overview of the clinical development path (i.e., request for conditional approval) and rationales
  Updates to Investigator’s Brochure for the next phase of development. (e.g., prior to First in Human include Core Safety Information from toxicology study)
  EXAMPLE OF DELIVERABLES FOR REVIEW
  
  Protocol synopsis
  Investigator Brochure
- - Criteria Clinical trial site feasibility completed
  TYPICAL ACTIVITIES
  
  Plan for site assessment (may include audit) including considerations such as infrastructure, capability, supply chain feasibility, capacity, etc.
  Understanding of required approval process to conduct clinical studies at all potential study sites and identifying risks
  EXAMPLE OF DELIVERABLES FOR REVIEW
  
  Summary report
- - Criteria Clinical vendors/ CRO identified and site initiation activities conducted
  TYPICAL ACTIVITIES
  
  Scope of work required (e.g., site selection, site initiation, data management, process & method development, etc.) and agreed metrics to monitor trial progress
  Partner engagement strategy (e.g., outsourced activity, insourced activity, consultation, etc.)
  Examples of past vaccine trial experience in the disease area/geographic area
  Understanding of the stepwise clinical trial approval process, engaging with local regulatory authorities, ethics committee etc.
  Existing network of investigators and study sites
  Audit record of clinical study sites and track record of staff GCP training
  Completion of site initiation activities
  EXAMPLE OF DELIVERABLES FOR REVIEW
  
  Summary report
- - Criteria Clinical assay readiness
  TYPICAL ACTIVITIES
  
  Relevant clinical assays need to be available prior to entering clinical studies
  EXAMPLE OF DELIVERABLES FOR REVIEW
  
  Summary of assay qualification
Study Start-up Activities Initiated
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GOALS/DEFINITIONS: Start-up activities are initiated to enable timely Phase 3 start. Clinical study start-up plan initiated with consideration of feasibility and identification of risks.
- - Criteria Clinical trial designed
  TYPICAL ACTIVITIES
  
  Protocol design and scope for the next phase of development (including study plans, medical monitoring plans, timelines and budgets) to support both NRA approval and WHO PQ
  Proposed clinical development path (i.e., request for conditional approval) and rationales
  Investigator’s Brochure updated for the next phase of development. (e.g., prior to First in Human include Core Safety Information from toxicology study)
  At EP2 ensure that feedback/recommendations from engagement with WHO (on target population etc.) are addressed in Phase 3 trial design
  EXAMPLE OF DELIVERABLES FOR REVIEW
  
  Phase 3 protocol and IB
- - Criteria Clinical trial site feasibility completed
  TYPICAL ACTIVITIES
  
  Plan for conducting epidemiology study to understand patient population and identifying potential study sites
  Existing network of investigators and study sites
  Plan for site validation (may include audit) including considerations such as infrastructure, capability, supply chain feasibility, capacity, cGCP certification, etc.
  Understanding of required approval process to conduct clinical studies at all potential study sites and identifying risks
  Data integrity and confidentiality practices
  EXAMPLE OF DELIVERABLES FOR REVIEW
  
  List of sites, risks and mitigations
- - Criteria Clinical vendors/CRO identified and site initiation activities conducted
  TYPICAL ACTIVITIES
  
  Scope of work required (e.g., site selection, site initiation, data management, process & method development, etc.) and agreed metrics to monitor trial progress
  Partner engagement strategy (e.g., outsourced activity, insourced activity, consultation, etc.)
  Relationship with local regulatory body, and authorities
  Existing network of investigators and study sites
  Ensure completion of site initiation activities such as:
  Plan for obtaining Ethical Committee approvals and completing all administrative tasks required to start a clinical study at all study sites;
  Plan for training of investigators and staff to ensure GCP compliance and protocol compliance (i.e., drug administration, dosing regimen, etc.);
  Plan for educating patients on protocol compliance (i.e., sample collection, adverse event reporting, etc.);
  Plan for obtaining Informed Consent with consideration of staff availability and patient literacy
  EXAMPLE OF DELIVERABLES FOR REVIEW
  
  Summary and start-up timelines
- - Criteria Clinical assay readiness
  TYPICAL ACTIVITIES
  
  Clinical lab identified
  Clinical assays in place prior to entering clinical studies
  EXAMPLE OF DELIVERABLES FOR REVIEW
  
  Summary of assay validation

Run Clinical Program Phase 1
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GOALS/DEFINITIONS: (1/2) Track clinical trial start date. Track the dosing of the first subject enrolled thereby indicating the beginning of the clinical trial. (2/2) Track Clinical Trial end date Track the date for the last subject to complete the trial thereby indicating the end of the clinical trial
- - (1/2) Criteria Track first dosing event for a patient recruited to the Phase 2 clinical trial
  TYPICAL ACTIVITIES
  
  Conduct recruitment analysis and compare study starts to the clinical plan
  Inform impact on other planned downstream activities in the case of study start delays
  EXAMPLE OF DELIVERABLES FOR REVIEW
  
  Notification of date first subject dosed and any delay, if incurred
- - (2/2) Criteria Track last patient to complete the Phase 2 clinical trial
  TYPICAL ACTIVITIES
  
  Conduct recruitment analysis and compare study duration to the clinical plan
  Inform impact on other planned downstream activities in the case of study completion delays
  EXAMPLE OF DELIVERABLES FOR REVIEW
  
  Notification of date last subject last visit and any delay, if incurred
Run Clinical Program Phase 2
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GOALS/DEFINITIONS: (1/4) Track clinical trial start date. Track the dosing of the first subject enrolled thereby indicating the beginning of the clinical trial. (2/4) Track that enrollment in the clinical trial is proceeding according to plan Track the progress and feasibility of Phase 3 clinical trials (3/4) Check that data quality is on track to meet target clinical study report date Monitor data cleaning process to expedite database lock, data analysis, and data submission (4/4) Track Clinical Trial end date Track the date for the last subject to complete the trial thereby indicating the end of the clinical trial
- - (1/4) Criteria Track first dosing event for a patient recruited to the Phase 3 clinical trial
  TYPICAL ACTIVITIES
  
  Conduct recruitment analysis and compare study starts to the clinical plan
  Inform impact on other planned downstream activities in the case of study start delays
  EXAMPLE OF DELIVERABLES FOR REVIEW
  
  Notification of date first subject dosed and any delay, if incurred
- - (2/4) Criteria Track recruitment and budget by comparing actual patient enrollment to previously established benchmarks at 25% of the projected recruitment period
  TYPICAL ACTIVITIES
  
  Conduct recruitment analysis and report number of patients recruited and budget within 25% of the projected recruitment period
  If suboptimal recruitment is identified, submit an analysis of recruitment barriers and a corrective recruitment plan with revised budget and timeline
  If recruitment levels are below minimum acceptable levels: evaluate feasibility to complete study within acceptable budget or timeframe and submit corrective recruitment plan
  EXAMPLE OF DELIVERABLES FOR REVIEW
  
  Notification of milestone achievement, any delay, mitigations and revised timeline
- - (3/4) Criteria Initiate data cleaning process as data becomes available to allow access to high integrity and quality data and expedite data analysis and submission
  - NOTE: Data cleaning process and plan should be clearly defined at the beginning of the study. Readiness for database lock should be considered at patient level and entire data base level.
  TYPICAL ACTIVITIES
  
  Streamlined data cleaning process to expedite clinical data analysis and submission
  Provide estimated time to database lock, data analysis, and data submission
  Report SAEs and any other issues
  EXAMPLE OF DELIVERABLES FOR REVIEW
  
  Notification of milestone achievement, any delay, mitigations and revised timeline
- - (4/4) Criteria Track last patient to complete the Phase 3 clinical trial
  TYPICAL ACTIVITIES
  
  Conduct recruitment analysis and compare study duration to the clinical plan
  Inform impact on other planned downstream activities in the case of study completion delays
  EXAMPLE OF DELIVERABLES FOR REVIEW
  
  Notification of date last subject last visit and any delay, if incurred
Run Clinical Program Phase 3
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GOALS/DEFINITIONS: (1/7) Track clinical trial start date. Track the dosing of the first subject enrolled thereby indicating the beginning of the clinical trial. (2/7) Track that enrollment in the clinical trial is proceeding according to plan. Track the progress and feasibility of Phase 3 clinical trials. (3/7) Check that data quality is on track to meet target clinical study report date. Monitor data cleaning process to expedite database lock, data analysis, and data submission. (4/7) Obtain an early read-out on the Phase 3 (if applicable) that may enable acceleration of regulatory submission. Phase 3 interim analysis completed (preferably by independent committees). (5/7) Track Clinical Trial end date. Track the date for the last subject to complete the trial thereby indicating the end of the clinical trial. (6/7) Leading indicator of availability of study analyses. Track the timing of database lock that informs the lag between the last subject dosed and the availability of study analyses. (7/7) Track availability of clinical trial data for decision making. Track the availability of top line results that enable real-time discussions of clinical trial data analysis and earlier investment decisions.
- - (1/7) Criteria Track first dosing event for a patient recruited to the Phase 3 clinical trial
  TYPICAL ACTIVITIES
  
  Conduct recruitment analysis and compare study starts to the clinical plan
  Inform impact on other planned downstream activities in the case of study start delays
  EXAMPLE OF DELIVERABLES FOR REVIEW
  
  Notification of date first subject dosed and any delay, if incurred
- - (2/7) Criteria Track recruitment and budget by comparing actual patient enrollment to previously established benchmarks at 25% of the projected recruitment period
  TYPICAL ACTIVITIES
  
  Conduct recruitment analysis and report number of patients recruited and budget within 25% of the projected recruitment period
  If suboptimal recruitment is identified, submit an analysis of recruitment barriers and a corrective recruitment plan with revised budget and timeline
  If recruitment levels are below minimum acceptable levels: evaluate feasibility to complete study within acceptable budget or timeframe and submit corrective recruitment plan
  EXAMPLE OF DELIVERABLES FOR REVIEW
  
  Notification of milestone achievement, any delay, mitigations and revised timeline
- - (3/7) Criteria Initiate data cleaning process as data becomes available to allow access to high integrity and quality data and expedite data analysis and submission
  - NOTE: Data cleaning process and plan should be clearly defined at the beginning of the study. Readiness for database lock should be considered at patient level and entire data base level.
  TYPICAL ACTIVITIES
  
  Streamlined data cleaning process to expedite clinical data analysis and submission
  Provide estimated time to database lock, data analysis, and data submission
  Report SAEs and any other issues
  EXAMPLE OF DELIVERABLES FOR REVIEW
  
  Notification of milestone achievement, any delay, mitigations and revised timeline
- - (4/7) Criteria Safety assessment completed
  TYPICAL ACTIVITIES
  
  Rate of severe adverse events (SAEs)
  EXAMPLE OF DELIVERABLES FOR REVIEW
  
  Interim clinical study report
- - (4/7) Criteria Efficacy assessment completed
  TYPICAL ACTIVITIES
  
  Statistically significant efficacy
  EXAMPLE OF DELIVERABLES FOR REVIEW
  
  As above
- - (4/7) Criteria Futility assessment (inability of trial to meet its objectives) completed
  TYPICAL ACTIVITIES
  
  Futility of trial effects (unlikely to achieve statistical significant efficacy)
  Operational futility (i.e., poor execution, lack of adequate resources, low adherence, poor quality of data)
  EXAMPLE OF DELIVERABLES FOR REVIEW
  
  As above
- - (4/7) Criteria Clinical trial strategy adjustment (if needed)
  TYPICAL ACTIVITIES
  
  Sample size re-adjustment
  Additional testing requirements
  EXAMPLE OF DELIVERABLES FOR REVIEW
  
  Updated IPDP
- - (4/7) Criteria TPP achievement assessed
  TYPICAL ACTIVITIES
  
  Probability assessment of whether candidate will meet target product profile
  EXAMPLE OF DELIVERABLES FOR REVIEW
  
  Use cTPP template
- - (5/7) Criteria Track last patient to complete the Phase 3 clinical trial
  TYPICAL ACTIVITIES
  
  Conduct recruitment analysis and compare study duration to the clinical plan
  Inform impact on other planned downstream activities in the case of study completion delays
  EXAMPLE OF DELIVERABLES FOR REVIEW
  
  Notification of date last subject last visit and any delay, if incurred
- - (6/7) Criteria Action taken to prevent further changes to the clinical trial database
  TYPICAL ACTIVITIES
  
  Database review and query resolution completed
  All pharmacokinetic, laboratory safety data and CRF data transferred to Data Management
  Database review and quality checks complete, data queries identified
  Query resolution completed
  EXAMPLE OF DELIVERABLES FOR REVIEW
  
  Notification of milestone achievement, any delay, mitigations and revised timeline
- - (7/7) Criteria Statistical analyses using preliminary or final data are completed
  TYPICAL ACTIVITIES
  
  Pharmacokinetic and pharmacodynamics (PK/PD) analyses of data completed
  Comparison of the observed results to the minimum criteria in the candidate TPP
  Working data sets delivered
  Tables, listings, figures produced to support topline report writing
  EXAMPLE OF DELIVERABLES FOR REVIEW
  
  Notification of milestone achievement, any delay, mitigations and revised timeline

Proof of Concept Obtained
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GOALS/DEFINITIONS: Data demonstrates that product has expected Mechanism of Action and has potential to meet cTPP. Drug candidate has demonstrated initial clinical efficacy Proof of Concept. (*Flexible milestone that may be evaluated at the end of phase 1, phase 2a, or phase 2b)
- - Criteria Clinical safety aligns with TPP criteria (includes clinical and laboratory abnormalities)
  TYPICAL ACTIVITIES
  
  Satisfactory safety profile using validated assays and adequate statistical analyses
  Safety signal detection (e.g., drug candidate-related adverse events (AEs) which may include serious adverse events (SAEs))
  Management of any adverse events (reporting of the events to the applicable ethical committees and regulatory agencies)
  EXAMPLE OF DELIVERABLES FOR REVIEW
  
  Summary of data and rationale
- - Criteria Efficacy proof-of-concept completed and aligns with TPP criteria
  TYPICAL ACTIVITIES
  
  Initial clinical efficacy proof-of-concept demonstrated using qualified/standardized clinical endpoint assays and adequate statistical analyses
  EXAMPLE OF DELIVERABLES FOR REVIEW
  
  Summary of data and rationale
- - Criteria Exposure-Response characterized to support selection of optimal dosage, regimen, and route of administration for Phase 2 trials defined
  TYPICAL ACTIVITIES
  
  Exposure-Response characterized
  Dose, regimen, and route of administration studies
  Recommendations for Phase 2 studies
  EXAMPLE OF DELIVERABLES FOR REVIEW
  
  Summary of data and rationale
- - Criteria TPP achievement assessed
  TYPICAL ACTIVITIES
  
  Probability assessment of whether candidate will meet target product profile
  EXAMPLE OF DELIVERABLES FOR REVIEW
  
  Use cTPP template
Proof of Concept Obtained * if not completed
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GOALS/DEFINITIONS: Data demonstrating Proof of Concept and that product and has potential to meet cTPP. Drug candidate has demonstrated initial clinical efficacy Proof of Concept. (*Flexible milestone that may be evaluated at the end of phase 1, phase 2a, or phase 2b)
- - Criteria Clinical safety aligns with TPP criteria (includes clinical and laboratory abnormalities)
  TYPICAL ACTIVITIES
  
  Satisfactory safety profile using validated assays and adequate statistical analyses
  Safety signal detection (e.g., drug candidate-related adverse events (AEs) which may include serious adverse events (SAEs))
  Management of any adverse events (reporting of the events to the applicable ethical committees and regulatory agencies)
  EXAMPLE OF DELIVERABLES FOR REVIEW
  
  Summary of data and rationale
- - Criteria Efficacy proof-of-concept completed and aligns with TPP criteria
  TYPICAL ACTIVITIES
  
  Initial clinical efficacy proof-of-concept demonstrated using qualified/standardized clinical endpoint assays and adequate statistical analyses
  Efficacy (either clinical disease or infection) in Phase 2a and/or Phase 2b studies in endemic populations
  Superiority or non-inferiority data in comparative studies against licensed drug (or treatment) control (if applicable)
  EXAMPLE OF DELIVERABLES FOR REVIEW
  
  Summary of data and rationale
- - Criteria Exposure-Response characterized to support selection of optimal dosage, regimen, and route of administration for Phase 3 trials defined
  TYPICAL ACTIVITIES
  
  Exposure-Response characterized
  Dose, regimen, and route of administration studies
  Recommendations for Phase 3 studies
  EXAMPLE OF DELIVERABLES FOR REVIEW
  
  Summary of data and rationale
- - Criteria TPP achievement assessed
  TYPICAL ACTIVITIES
  
  Probability assessment of whether candidate will meet target product profile
  EXAMPLE OF DELIVERABLES FOR REVIEW
  
  Use cTPP template

Clinical Development Plan in Place
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GOALS/DEFINITIONS: Detailed plan for Phase 1 and high level plan for Phase 2 and 3 in place. Clinical Development Plan initiated. (*Clinical Development Plan is initiated prior to the FIH gate review and is updated & reviewed during development through to the DTF gate review)
- - Criteria Clinical development plan initiated
  TYPICAL ACTIVITIES
  
  Overview of planned clinical activities:
  Study phase, objectives / research rationale
  Duration of the studies, number of subjects, recruitment criteria (e.g.,. study arms, patient cohorts, comparators for non-inferiority trials, power calculations etc.)
  Dosing & dosing modeling strategies
  Detailed rationale for Phase 1 dose range, and target clinical exposures
  Toxicology and toxicokinetic results to support doses and dosing duration in Phase 2
  Drug combination assessment & plan
  Toxicology plan to support Phase 2
  Clinical partners, proposed target countries, and study sites (based on criteria including clinical expertise, sustainability, site capacity, and disease incidence / epidemiology studies, etc.)
  Definition of clinical endpoints (primary & secondary), methodology (clinical endpoint assays, data collection plan, statistical methods, etc.), adverse event reporting, stopping rules, etc.
  Monitoring, data management, and biostatistics strategies
  Post-marketed product surveillance / Phase 4 trial strategy
  Mass product administration considerations (e.g., trial design, safety requirements, etc.)
  Off-label use considerations
  Trial size considerations for diseases with limited incidence rates
  Potential risks and mitigation strategies
  Timelines and budgets for clinical development
  EXAMPLE OF DELIVERABLES FOR REVIEW
  
  Detailed plan with timeline for Phase 1
  High-level / draft plan for Phase 2 and Phase 3 risk identification and mitigation
  Plans should reflect approaches to accelerate decision making (e.g., adaptive designs, real-time data analysis of clinical trials etc.)
  Phase 2 plan is modified during
  Phase 1 trial as Phase 1 data become available
  Clinical development plan extends beyond DTF to accommodate the time needed to report Phase 3 results and also cover additional plans for pediatric studies and post-market surveillance
Clinical Development Plan Updated
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GOALS/DEFINITIONS: Clinical safety data and rationale for Phase 2 dose selection. Clinical Development Plan initiated. (*Clinical Development Plan is initiated prior to the FIH gate review and is updated & reviewed during development through to the DTF gate review)
- - Criteria Clinical development plan updated
  TYPICAL ACTIVITIES
  
  Overview of planned clinical activities:
  Study phase, objectives / research rationale
  Duration of the studies, number of subjects, recruitment criteria (e.g.,. study arms, patient cohorts, comparators for non-inferiority trials, power calculations etc.)
  Dosing & dosing modeling strategies
  Detailed rationale for Phase 2 dose range, and target clinical exposures
  Toxicology and toxicokinetic results to support doses and dosing duration in Phase 2
  Drug combination assessment & plan
  Toxicology plan to support Phase 3
  Clinical partners, proposed target countries, and study sites (based on criteria including clinical expertise, sustainability, site capacity, and disease incidence / epidemiology studies, etc.)
  Definition of clinical endpoints (primary & secondary), methodology (clinical endpoint assays, data collection plan, statistical methods, etc.), adverse event reporting, stopping rules, etc.
  Monitoring, data management, and biostatistics strategies
  Post-marketed product surveillance / Phase 4 trial strategy
  Mass product administration considerations (e.g., trial design, safety requirements, etc.)
  Off-label use considerations
  Trial size considerations for diseases with limited incidence rates
  Potential risks and mitigation strategies
  Timelines and budgets for clinical development
  EXAMPLE OF DELIVERABLES FOR REVIEW
  
  Detailed Phase 2 clinical plan with timeline including supporting CMC and tox plans
  High-level / draft plan for Phase 3
  Updated risk identification and mitigation needed for all subsequent phases of development
  Plans should reflect approaches to accelerate decision making (e.g., adaptive designs, real-time data analysis of clinical trials etc.)
  Phase 2 plan is modified during Phase 1 trial as Phase 1 data become available
  Clinical development plan extends beyond DTF to accommodate the time needed to report Phase 3 results and also cover additional plans for pediatric studies and post-market surveillance
Clinical Development Plan Updated
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GOALS/DEFINITIONS: Plan for clinical studies for licensure and post-marketing. Clinical Development Plan initiated. (*Clinical Development Plan is initiated prior to the FIH gate review and is updated & reviewed during development through to the DTF gate review)
- - Criteria Clinical development plan updated
  TYPICAL ACTIVITIES
  
  Overview of planned clinical activities:
  Study phase, objectives/research rationale
  Duration of the studies, number of subjects, recruitment criteria (e.g.,. study arms, patient cohorts, comparators for non-inferiority trials, power calculations etc.)
  Complete drug-drug interaction and special population place in place
  Dosing & dosing modeling strategies
  Detailed rationale for Phase 3 dose selection
  Toxicology and toxicokinetic results to support doses and dosing duration in Phase 3
  Drug combination assessment & plan
  Toxicology plan to support submission (e.g., carcinogenicity, reproductive toxicology)
  Clinical partners, proposed target countries, and study sites (based on criteria including clinical expertise, sustainability, site capacity, and disease incidence/epidemiology studies, etc.)
  Definition of clinical endpoints (primary & secondary), methodology (clinical endpoint assays, data collection plan, statistical methods, etc.), adverse event reporting, stopping rules, etc.
  Monitoring, data management, and biostatistics strategies
  Post-marketed product surveillance/Phase 4 trial strategy
  Mass product administration considerations (e.g., trial design, safety requirements, etc.)
  Off-label use considerations
  Trial size considerations for diseases with limited incidence rates
  Potential risks and mitigation strategies
  Timelines and budgets for clinical development
  EXAMPLE OF DELIVERABLES FOR REVIEW
  
  Detailed Phase 3 clinical plan with timeline
  Updated risk identification and mitigation needed for all subsequent phases of development
  Plans should reflect approaches to accelerate decision making (e.g., adaptive designs, real-time data analysis of clinical trials etc.)
  Phase 3 plan is modified during
  Phase 2 trial as Phase 2 data become available
  Clinical development plan extends beyond DTF to accommodate the time needed to report Phase 3 results and also cover additional plans for pediatric studies and post-market surveillance
Clinical Development Plan Updated
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GOALS/DEFINITIONS: Clinical safety data and rationale for registration. Clinical Development Plan initiated. (*Clinical Development Plan is initiated prior to the FIH gate review and is updated & reviewed during development through to the DTF gate review)
- - Criteria Clinical development plan initiated
  TYPICAL ACTIVITIES
  
  Overview of planned clinical activities post-approval:
  Study phase, objectives/research rationale
  Duration of the studies, number of subjects, recruitment criteria (e.g.,. study arms, patient cohorts, comparators for non-inferiority trials, power calculations etc.)
  Special populations dosing & dosing modeling strategies
  New formulation assessment & plan
  Clinical partners, proposed target countries, and study sites (based on criteria including clinical expertise, sustainability, site capacity, and disease incidence/epidemiology studies, etc.)
  Post-marketed product surveillance/Phase 4 trial strategy
  Mass product administration considerations (e.g., trial design, safety requirements, etc.)
  Off-label use considerations
  Trial size considerations for diseases with limited incidence rates
  Potential risks and mitigation strategies
  Timelines and budgets for post-approval clinical development
  EXAMPLE OF DELIVERABLES FOR REVIEW
  
  Detailed post approval clinical plan with timeline
  Risk identification and mitigation needed for post approval phase of development
  Post approval Clinical Development Plan should be finalized prior to the DTF gate review (i.e., prior to registration)
  Clinical Development Plan extends beyond DTF gate to accommodate time needed to report Phase 3 results and also to cover additional plans for pediatric studies and post-market surveillance
  * Items in bold font reflect suggested reporting guidelines for this stage gate

Phase 1 Endpoints Met
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GOALS/DEFINITIONS: Human safety and dose established. Phase 1 endpoints met.
- - Criteria Initial safety and tolerability demonstrated (no gross clinical and laboratory abnormalities) relative to the TPP
  TYPICAL ACTIVITIES
  
  Satisfactory safety profile using validated methods and adequate statistical analyses:
  Drug-related adverse events (AEs) which may include serious adverse events (SAEs)
  Management of any adverse events (reporting of the events to the applicable ethical committees and regulatory agencies)
  EXAMPLE OF DELIVERABLES FOR REVIEW
  
  Summary of clinical safety data, AEs and SAEs
- - Criteria Phase 1 safety, pharmacokinetics and biomarker data do not preclude the further development of the compound relative to the TPP
  TYPICAL ACTIVITIES
  
  Validated bioanalytical measurements of drug candidate exposure and relevant biomarker concentrations
  Preliminary exposure-response relationships based on biomarker data
  EXAMPLE OF DELIVERABLES FOR REVIEW
  
  Summary of clinical PK data, exposure, half life and recommended Phase 2 dose with rationale
Phase 3 Endpoints Met
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GOALS/DEFINITIONS: Safety, efficacy, and desired outcomes in humans demonstrated in pivotal trial. Safety, efficacy, and desired outcomes in humans (full analysis) demonstrated.
- - Criteria Safety (includes clinical and laboratory abnormalities) profile of candidate aligns with TPP
  TYPICAL ACTIVITIES
  
  Satisfactory safety profile using validated clinical endpoint assays and adequate statistical analyses:
  Safety signal detection (e.g., adverse events (AEs) which may include serious adverse events (SAEs))
  Fully characterized drug-drug interactions
  Management of any adverse events (reporting of the events to the applicable ethical committees and regulatory agencies)
  EXAMPLE OF DELIVERABLES FOR REVIEW
  
  Summary of Phase 3 clinical trial data
- - Criteria Efficacy profile of candidate aligns with TPP
  TYPICAL ACTIVITIES
  
  Clinical efficacy demonstrated using validated clinical endpoint assays and adequate statistical analyses:
  Sufficient efficacy duration to achieve impact
  Superiority or non-inferiority data in comparative studies against licensed drug (or treatment) control (if applicable)
  EXAMPLE OF DELIVERABLES FOR REVIEW
  
  Summary of Phase 3 clinical trial data
- - Criteria Other TPP characteristics met
  TYPICAL ACTIVITIES
  
  Assessment of whether candidate meets target product profile
  EXAMPLE OF DELIVERABLES FOR REVIEW
  
  Use cTPP template

Business Case Updated
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GOALS/DEFINITIONS: Business case for developing a deliverable product Business Case, Deliverability Assessment, Strategic Demand Forecast and COGS reports and Cost Effectiveness Report
- - Criteria Business Case
  TYPICAL ACTIVITIES
  
  Business case provides overview of product candidate’s strategic value and market viability, including:
  Value proposition against foundation’s disease strategy and other interventions in market
  Estimate of overall costs to launch and drive uptake
  Summary of market understanding (e.g., size, segments, user needs, etc.)
  EXAMPLE OF DELIVERABLES FOR REVIEW
  
  Provide key assumptions and rationale for business case
Business Case
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GOALS/DEFINITIONS: Business Case for developing a deliverable product Business Case, Deliverability Assessment, Strategic Demand Forecast and COGS reports and Cost Effectiveness Report
- - Criteria Business Case
  TYPICAL ACTIVITIES
  
  Business case provides overview of product candidate’s strategic value and market viability, including:
  Value proposition against foundation’s disease strategy and other interventions in market
  Estimate of overall costs to launch and drive uptake
  Summary of market understanding (e.g., size, segments, user needs, etc.)
  EXAMPLE OF DELIVERABLES FOR REVIEW
  
  Provide key assumptions and rationale for business case
Coverage and Financial Tracker
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GOALS/DEFINITIONS: Business Case for developing a deliverable product Business Case, Deliverability Assessment, Strategic Demand Forecast and COGS reports and Cost Effectiveness report
- - Criteria Coverage and Financial Tracker
  TYPICAL ACTIVITIES
  
  The first iteration of the coverage and financial tracker should:
  Develop target metrics for number of countries launched, coverage, average procurement price, and incremental costs to deliver
  *At PQ / LR these metrics should be refined.
  EXAMPLE OF DELIVERABLES FOR REVIEW
  
  Draft target metrics
Global Normative Guidance
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GOALS/DEFINITIONS: Date when critical normative guidance (country adoption into national guidelines if in a single focal country, WHO policy guidance, SAGE recommendation, other) is announced publicly.

Deliverability Assessment
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GOALS/DEFINITIONS: Business Case for developing a deliverable product Business Case, Deliverability Assessment, Strategic Demand Forecast and COGS reports and Cost Effectiveness Report
- - Criteria Deliverability Assessment
  TYPICAL ACTIVITIES
  
  A deliverability assessment will provide a high-level assessment of risks and opportunities for:
  Improvement relative to standard of care
  Considerations around the global and country awareness of the intervention, possibility of financing,
  Global policy and regulatory pathway
  Supply chain and user targeting
  Frequency and mode of delivery and any special handling required
  Novelty relative to existing products
  Manufacturing considerations
  Provider-related issues including workflow and training (ex: maintenance and calibration)
  Patient access, perception of value and economics
  Disease risk awareness in population
  EXAMPLE OF DELIVERABLES FOR REVIEW
  
  Summary report
Deliverability Assessment Updated
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GOALS/DEFINITIONS: Business case for developing a deliverable product Business Case, Deliverability Assessment, Strategic Demand Forecast and COGS reports and Cost Effectiveness Report
- - Criteria Deliverability Assessment
  TYPICAL ACTIVITIES
  
  A deliverability assessment will provide a high-level assessment of risks and opportunities for:
  Improvement relative to standard of care
  Considerations around the global and country awareness of the intervention, possibility of financing,
  Global policy and regulatory pathway
  Supply chain and user targeting
  Frequency and mode of delivery and any special handling required
  Novelty relative to existing products
  Manufacturing considerations
  Provider-related issues including workflow and training (ex: maintenance and calibration)
  Patient access, perception of value and economics
  Disease risk awareness in population
  EXAMPLE OF DELIVERABLES FOR REVIEW
  
  Summary report
Deliverability Assessment Updated
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GOALS/DEFINITIONS: Business case for developing a deliverable product Identification of commercial partner(s) for launch and full-scale manufacturing of the product
- - Criteria Deliverability Assessment
  TYPICAL ACTIVITIES
  
  The delivery plan will summarize:
  Regulatory plan and first-wave country partners
  Production/manufacturing partners with projected product price, volume, and revenue
  Country supply chain and user targeting methodology
  Roll-out plans for first-wave countries
  Country decision support plans that verify capacity, resources, and new technologies for introduction
  Global policy and initiative opportunities/partnerships
  Benefits over current standard of care
  Global policy milestones and pathway identified to reach critical registration (i.e., PQ, EMA)
  EXAMPLE OF DELIVERABLES FOR REVIEW
  
  Summary report

Launch Budget Prediction Updated
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GOALS/DEFINITIONS: Business Case for developing a deliverable product Business Case, Deliverability Assessment, Strategic Demand Forecast and COGS reports and Cost Effectiveness report
- - Criteria Launch Budget Prediction
  TYPICAL ACTIVITIES
  
  The refined launch budget prediction will provide:
  A detailed and accurate estimation of the scale of launch support and budget for successful uptake
  EXAMPLE OF DELIVERABLES FOR REVIEW
  
  Refined launch budget
Launch Budget Prediction
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GOALS/DEFINITIONS: Business case for developing a deliverable product Identification of commercial partner(s) for launch and full-scale manufacturing of the product
- - Criteria Launch Budget Prediction
  TYPICAL ACTIVITIES
  
  The first iteration of the launch budget prediction will include:
  An estimate of the scale of launch support and budget for successful uptake
  Detailed budget for pre-launch activities
  EXAMPLE OF DELIVERABLES FOR REVIEW
  
  Draft launch budget
Launch in First Country
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:

Strategic Demand Forecast
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GOALS/DEFINITIONS: Business Case for developing a deliverable product Business Case, Deliverability Assessment, Strategic Demand Forecast and COGS reports and Cost Effectiveness Report
- - Criteria Strategic Demand Forecast
  TYPICAL ACTIVITIES
  
  Methodology to be used to assess potential demand adjusted for product availability, country introduction decisions, uptake timing (without any supply or financing constraints)
  DONOR provides a methodology grantees may use for demand forecasting
  Demand forecast methods should align with to the DONOR valuation model (in Integrated Portfolio Management tool)
  EXAMPLE OF DELIVERABLES FOR REVIEW
  
  DONOR provides methodology
Strategic Demand Forecast Updated
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GOALS/DEFINITIONS: Business case for developing a deliverable product Business Case, Deliverability Assessment, Strategic Demand Forecast and COGS reports and Cost Effectiveness Report
- - Criteria Strategic Demand Forecast
  TYPICAL ACTIVITIES
  
  An initial, high-level demand forecast will identify:
  Target countries
  Target sub populations
  Timing of introduction specific to identified countries
  EXAMPLE OF DELIVERABLES FOR REVIEW
  
  DONOR provides methodology
Strategic Demand Forecast Updated
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GOALS/DEFINITIONS: Business case for developing a deliverable product Identification of commercial partner(s) for launch and full-scale manufacturing of the product
- - Criteria Strategic Demand Forecast
  TYPICAL ACTIVITIES
  
  The demand forecast at EP2 will include:
  Target countries for introduction
  Target populations/sub-populations
  Timing and speed of introduction specific to identified countries
  Product accessibility and availability
  Predicted coverage rate
  Expected volumes and pricing
  Sensitivity analysis based on key assumptions and drivers of forecast
  EXAMPLE OF DELIVERABLES FOR REVIEW
  
  DONOR provides methodology
Strategic Demand Forecast Updated
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GOALS/DEFINITIONS: Business Case for developing a deliverable product Business Case, Deliverability Assessment, Strategic Demand Forecast and COGS reports and Cost Effectiveness report
- - Criteria Strategic demand Forecast
  TYPICAL ACTIVITIES
  
  The demand forecast will include refined iterations of:
  Target countries for introduction
  Target populations/sub-populations
  Timing and speed of introduction specific to identified countries
  Product accessibility and availability
  Predicted coverage rate
  Expected volumes and pricing
  Sensitivity analysis based on key assumptions and drivers of forecast
  EXAMPLE OF DELIVERABLES FOR REVIEW
  
  DONOR provides methodology
50% Coverage Achieved
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GOALS/DEFINITIONS: Date when anticipate achieving 50% of the program strategy team’s coverage goal for the overall product class (see below) – i.e., if the goal for rotavirus vaccines is 80% coverage in Gavi countries, then year X is when coverage is expected to achieve the half-way point (40% coverall in all, or 80% in half of Gavi countries); if the target is 20m male circumcisions in target geographies, then year Y when coverage is expected to achieve the half-way point (10m). Product class is defined as the general category that is the next order up from the candidate or product name. This is likely to align with how coverage tracked for a health intervention. Examples are rotavirus vaccine, HIV first-line drug, TB molecular diagnostic, etc. Please specify the product class in the “Target Coverage/Market Share Description” field.

COGS
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GOALS/DEFINITIONS: Business Case for developing a deliverable product Business Case, Deliverability Assessment, Strategic Demand Forecast and COGS reports and Cost Effectiveness Report
- - Criteria COGS
  TYPICAL ACTIVITIES
  
  Methodology to be used to build up COGS over the course of product development
  During FIH, an initial aspirational COGS should be set to drive TPP and goals for projected costs related to the product
  EXAMPLE OF DELIVERABLES FOR REVIEW
  
  DONOR provides methodology
COGS Updated
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GOALS/DEFINITIONS: Business case for developing a deliverable product. Business Case, deliverability assessment, strategic demand forecast and COGS reports completed.
- - Criteria COGS
  TYPICAL ACTIVITIES
  
  An initial, high-level COGS analysis at EP1 will identify:
  Key cost drivers
  Cost estimate assumptions for equipment needed, processes
  Projected price (within 30% of TPP target)
  EXAMPLE OF DELIVERABLES FOR REVIEW
  
  DONOR provides methodology
COGS Updated
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GOALS/DEFINITIONS: Business case for developing a deliverable product Identification of commercial partner(s) for launch and full-scale manufacturing of the product
- - Criteria COGS
  TYPICAL ACTIVITIES
  
  A COGS analysis at EP2 will identify:
  Product price, volume, and revenue based on commercial scale production
  Variable and fixed costs for R&D, facilities, equipment, labor, and raw materials
  Licensing expenses and incomes
  Grants, loans and outstanding debts related to the product
  Related product sales
  Projected price (within 30% of TPP target)
  EXAMPLE OF DELIVERABLES FOR REVIEW
  
  DONOR provides methodology
COGS Updated
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GOALS/DEFINITIONS: Business Case for developing a deliverable product Business Case, Deliverability Assessment, Strategic Demand Forecast and COGS reports and Cost Effectiveness report
- - Criteria COGS
  TYPICAL ACTIVITIES
  
  The COGS analysis will include refined iterations of:
  Product price, volume, and revenue based on commercial scale production
  Variable and fixed costs (for all areas in COGS methodology)
  Licensing expenses and incomes
  Grants, loans and outstanding debts related to the product
  Related product sales
  Expected price, aligned with TPP & DONOR strategy
  Initial allocation and partner negotiation around shared and indirect costs
  EXAMPLE OF DELIVERABLES FOR REVIEW
  
  DONOR provides methodology
Target Market Share Achieved
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GOALS/DEFINITIONS: Date when anticipate this specific product will achieve the target market share for the overall product class – i.e., Year X when Gene X-pert will represent 25% market share of all TB molecular diagnostics. This should be informed by a demand forecast and initially should mirror the assumptions made for impact modeling and should be refined over time with more concrete demand forecasts. Please leave blank if the team is agnostic as to coverage of the specific product and is more interested in overall coverage of the product class or if this is the only product class or if the team has not yet thought through these questions.

Cost-Effectiveness Analysis
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GOALS/DEFINITIONS: Business Case for developing a deliverable product Business Case, Deliverability Assessment, Strategic Demand Forecast and COGS reports and Cost Effectiveness Report
- - Criteria Cost-Effectiveness Analysis
  TYPICAL ACTIVITIES
  
  Methodology to be used to assess drivers of health and economic outcomes and interventions/product candidates
  DONOR provides a methodology grantees may use for cost-effectiveness analysis
  Cost-effectiveness methods should align with to the DONOR valuation model (in Integrated Portfolio Management tool)
  EXAMPLE OF DELIVERABLES FOR REVIEW
  
  DONOR provides methodology
Cost-Effectiveness Analysis Updated
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GOALS/DEFINITIONS: Business Case for developing a deliverable product Business Case, Deliverability Assessment, Strategic Demand Forecast and COGS reports and Cost Effectiveness Report
- - Criteria Cost-Effectiveness Analysis
  TYPICAL ACTIVITIES
  
  An initial, high-level cost-effectiveness analysis will identify:
  Anticipated health and economic benefits of the product
  Projected health and economic costs to achieve the benefits
  Comparisons to existing standards of care
  EXAMPLE OF DELIVERABLES FOR REVIEW
  
  DONOR provides methodology
Cost-Effectiveness Analysis Updated
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GOALS/DEFINITIONS: Business case for developing a deliverable product Identification of commercial partner(s) for launch and full-scale manufacturing of the product
- - Criteria Cost-Effectiveness Analysis
  TYPICAL ACTIVITIES
  
  A cost-effectiveness analysis at EP2 will identify:
  Limitations of economic evaluations performed
  Comparators and mean costs and effects of the product and the competitor
  Cost and effects of the product on sub-populations
  Groups that may be disproportionally impacted positively or negatively
  EXAMPLE OF DELIVERABLES FOR REVIEW
  
  DONOR provides methodology
Cost-Effectiveness Analysis Updated
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GOALS/DEFINITIONS: Business Case for developing a deliverable product Business Case, Deliverability Assessment, Strategic Demand Forecast and COGS reports and Cost Effectiveness report
- - Criteria Cost-effectiveness analysis
  TYPICAL ACTIVITIES
  
  The cost-effectiveness analysis will include refined iterations of:
  Limitations of economic evaluations performed
  Comparators and mean costs and effects of the product and the competitor
  Cost and effects of the product on sub-populations
  Groups that may be disproportionally impacted positively or negatively
  Note: Additional inputs expected from Delivery team
  EXAMPLE OF DELIVERABLES FOR REVIEW
  
  DONOR provides methodology

CMOs/CROs selected
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GOALS/DEFINITIONS: (1/2) Rationale and justification for selection of drug development partners Drug development service providers engaged and qualified (*Partner Selection may be competed prior to either the PCD or FIH gate reviews, depending on specific-product requirements) (2/2) Rationale and justification for selection of drug development partners Drug development service providers engaged and qualified (*Partner Selection may be competed prior to either the PCD or FIH gate reviews, depending on specific-product requirements)
- - (1/2) Criteria Contract research partners (to facilitate / enable preclinical process development) engaged and qualified
  TYPICAL ACTIVITIES
  
  Scope of work required (e.g., functional activities, process & method development, etc.)
  Partner engagement strategy (e.g., outsourced activity, insourced activity, consultation, etc.)
  cGLP certification
  Audits by FDA / NRAs and client
  Confirmation of capabilities, equipment, equipment qualification & process/method validation packages, staff training, SOPs, etc.
  Previous experience with partner (e.g., successes & failures)
  Preliminary cost information
  Lead times/time in the queue
  Contract terms and long-term contingencies
  EXAMPLE OF DELIVERABLES FOR REVIEW
  
  Summary of key data and rationale to support partner selection
  Additional detail may be reported in an appendix
- - (2/2) Criteria Contract manufacturing partners (to facilitate / enable clinical supply) engaged and qualified
  - * CMC experts should be engaged to assess partners for drug substance, drug product manufacturing and analytical services
  TYPICAL ACTIVITIES
  
  Scope of work required (e.g., functional activities, process & method development, etc.)
  Partner engagement strategy (e.g., outsourced activity, insourced activity, consultation, etc.)
  cGMP certification
  Audits by FDA / NRAs and client
  Confirmation of capabilities, capacity, quality control systems, equipment, equipment qualification & process/method validation packages, staff training, SOPs, etc.
  Previous experience with partner (e.g., successes & failures)
  Preliminary cost information
  Lead times / time in the queue
  Contract terms and long-term contingencies
  EXAMPLE OF DELIVERABLES FOR REVIEW
  
  Summary of key data and rationale to support partner selection
  Additional detail may be reported in an appendix
- - (2/2) Criteria Support service partners (e.g., to enable initial regulatory requirements, file patents, provide legal counsel, etc.) engaged and qualified
  TYPICAL ACTIVITIES
  
  Scope of work required (e.g., IND preparation, patent creation, legal counsel, etc.)
  Partner engagement strategy (e.g., outsourced activity, insourced activity, consultation, etc.)
  Confirmation of capabilities & services
  Previous experience with partner (e.g., successes & failures)
  Preliminary cost information
  Lead times / time in the queue
  EXAMPLE OF DELIVERABLES FOR REVIEW
  
  Summary of key data and rationale to support partner selection
  Additional detail may be reported in an appendix
Partner Selection Plan in Place
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GOALS/DEFINITIONS: Determine need for product development partner and plan for partner selection. Partnership requirements plan completed.
- - Criteria Partnership requirements identified (high level)
  TYPICAL ACTIVITIES
  
  Analysis to decide whether there is need to partner for product development to complement internal capabilities across all stages of drug development, which could include:
  Functional activity partners such as CROs, CMOs, commercial biopharmaceutical companies, PDPs & out-licensers needed for discovery, preclinical & clinical development, manufacturing, delivery/uptake, etc.
  Supporting activity partners such as IP, Legal, Regulatory, Global Access, etc. Firms/Agencies
  Partner capability requirement
  Potential partner shortlist
  EXAMPLE OF DELIVERABLES FOR REVIEW
  
  List of internal capabilities and identified gaps
- - Criteria Path & timing for partnership engagement identified (high level)
  TYPICAL ACTIVITIES
  
  Partnership engagement path (e.g., DONOR network, academia, service providers)
  Timing and length of partnership engagements
  EXAMPLE OF DELIVERABLES FOR REVIEW
  
  Up to one page description of partner engagement plan
- - Criteria Anticipated partnership challenges and risks identified (high level)
  TYPICAL ACTIVITIES
  
  Anticipated challenges, risks, and contingencies for product development
  Mitigation plan and trigger mechanisms
  EXAMPLE OF DELIVERABLES FOR REVIEW
  
  Table summarizing risk, probability of occurrence, potential impact and mitigations
Commercial Partner Identified * if not completed
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GOALS/DEFINITIONS: Rationale and justification for selection of commercial partner. Identification of commercial partner(s) for launch and full-scale manufacturing of the product.
- - Criteria Partner (commercial, government, non-profit, etc.) assessments to determine the fit for collaboration completed
  TYPICAL ACTIVITIES
  
  Respective expectations and business model (i.e., pricing of drug pricing upon licensure, IP control, etc.)
  Mid- to long-term strategic fit (i.e., intent for pursuit of the product over mid/long term to ensure the viability of the product development and partnership)
  Assess whether the NRA in the manufacturer’s country is considered a functional NRA by the WHO
  Identify timing of decision points where contingency plan needs to be triggered if suitable commercial partner is not selected
  EXAMPLE OF DELIVERABLES FOR REVIEW
  
  Summary of key data and rationale to support partner selection
  Additional detail may be reported in an appendix
Commercial Partner Identified
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GOALS/DEFINITIONS: Rationale and justification for selection of commercial partner. Identification of commercial partner(s) for launch and full-scale manufacturing of the product.
- - Criteria Partner (commercial, government, non-profit, etc.) assessments to determine the fit for collaboration completed
  TYPICAL ACTIVITIES
  
  Respective expectations and business model (i.e., pricing of drug pricing upon licensure, IP control, etc.)
  Mid- to long-term strategic fit (i.e., intent for pursuit of the product over mid/long term to ensure the viability of the product development and partnership)
  Assess whether the NRA in the manufacturer’s country is considered a functional NRA by the WHO
  Identify timing of decision points where contingency plan needs to be triggered if suitable commercial partner is not selected
  EXAMPLE OF DELIVERABLES FOR REVIEW
  
  Summary of key data and rationale to support partner selection
  Additional detail may be reported in an appendix

Lead Chemical Series Selected

Lead Optimization Completed

IND-Enabling Studies Completed

Candidate Target Product Profile Expectations

Updated Candidate TPP

Updated Candidate TPP

Updated Candidate TPP

CMC Development Plan In Place (Drugs)

CMC Development Plan Updated (Drugs)

CMC Development Plan Updated (Drugs)

CMC Development Plan Updated (Drugs)

CMC Development Plan Updated (Drugs)

Initial DS/DP Characterization Complete

DS/DP Characterized at Kilo-Scale