3.3 Formal qualification programs

Overview

Formal qualification is a voluntary process that results in FDA’s endorsement of a measure or tool for a specific context of use. Once qualified, the tool can be used by any sponsor for that qualified purpose without FDA needing to re-review its suitability. The [MDDT] (Medical Device Development Tool) and [DDT] (Drug Development Tool) qualification programs operate as an overlay on top of (not substituting for) the existing drug and device regulatory pathways, rather than as standalone approval pathways. Additionally, some, but not all, sDHTs may fall under the ISTAND program (which is part of the DDT program).

Evaluate drug, device, or combination product pathways for the medical product itself, and consider tool-specific qualification pathways when your sDHT is intended for reuse across programs within a defined context of use.

Qualification is not required for most sDHT applications

If you’re using an sDHT-derived endpoint in a single development program, you can establish its fitness through your product-specific regulatory interactions. Qualification is a valuable option when:

The measure addresses a broadly applicable need across multiple sponsors or therapeutic programs

You want to reduce duplicative evidence generation across the field

You’re building a tool intended for widespread adoption and want formal regulatory endorsement to support that goal

Two primary qualification pathways exist

Before pursuing qualification, ask:

Is the measure intended for use beyond a single development program?

Is there unmet need in the field that qualification would address?

Do you have (or can you generate) sufficient evidence to meet the evidentiary bar?

Are you prepared for a multi-year process?

If the answer to any of these is “no,” product-specific engagement (covered in Section 3.2: Pathway selection & timing) may be more appropriate.

in practice

3.3B DDT Qualification Program

The Drug Development Tool (DDT) Qualification Program provides pathways for FDA to formally qualify tools—including sDHT-derived measures—that drug and biologic sponsors can rely upon in their development programs.

What qualifies as a DDT?

DDTs include biomarkers, clinical outcome assessments (COAs), and animal models. For sDHTs, the relevant pathways are typically:

Clinical Outcome Assessment (COA) Qualification: For sDHT-derived measures that capture how a patient feels, functions, or survives

Biomarker Qualification: For sDHT-derived measures that indicate a biological process, disease state, or response to treatment

What does qualification mean?

“Qualification is a conclusion that within the stated context of use, the DDT can be relied upon to have a specific interpretation and application in drug development and regulatory review. Once qualified, DDTs will be publicly available to be used in any drug development program for the qualified context of use. Additionally, the qualified DDT generally can be included in IND, NDA, or BLA submissions without needing FDA to reconsider and reconfirm its suitability.”

– Drug Development Tool (DDT) Qualification Programs, FDA, 2025

When to consider DDT qualification

DDT qualification may be appropriate when:

DDT qualification is likely not the right path if:

DDT program snapshot

As of June 2025, the program has qualified 17 tools overall: 8 biomarkers, 8 COAs, and 1 animal model. With 141 projects in development (including 67 for COAs and 59 for biomarkers), the program reflects growing interest.

Timelines vary but can span several years; COA qualifications have historically averaged around 6 years, though recent guidance aims to streamline processes. No sDHTs have been fully qualified through the FDA’s Drug Development Tool (DDT) qualification program as of late 2025; however, Sibel Health’s nocturnal scratch digital endpoint, submitted in collaboration with partners, is currently under review as a DDT for atopic dermatitis trials.

Visit FDA’s DDT qualification project database to search across DDT qualification programs by stage of submission, qualification status, disease, and therapeutic area.

fda spotlight

“Mission and Objectives of the DDT Qualification Programs:

• To qualify and make DDTs publicly available for a specific context of use to expedite drug development and review of regulatory applications

• To provide a framework for early engagement and scientific collaboration with FDA to facilitate DDT development

• To facilitate integration of qualified DDTs in regulatory review

• To encourage development of DDTs for contexts of use with unmet needs

• To encourage the formation of collaborative groups to undertake DDT development programs to increase the efficiency and lessen the individual resource burden incumbent with DDT development

• To encourage innovation in drug development

• To create a shared learning environment for exchanging information on DDT development”

Drug Development Tool (DDT) Qualification Programs

Drug Development Tool (DDT) Qualification Programs

2025 FDA

FDA – informational resource

Authors

FDA

This FDA webpage provides a comprehensive overview of the Drug Development Tool (DDT) Qualification Programs. It serves as a central resource for stakeholders—including drug developers, academic researchers, and patient organizations—to understand the formal process for qualifying DDTs for a specific context of use. The page outlines the three main qualification programs: the Biomarker Qualification Program, the Clinical Outcome Assessment (COA) Qualification Program, and the Animal Model Qualification Program. The overall mission is to streamline drug development by creating a clear pathway for the validation and acceptance of innovative tools that can be publicly used across multiple development programs.

Key Principles (Findings)
The central principle of the DDT Qualification Programs is to create a formal pathway for the FDA to conclude that a specific tool is well-suited for a particular Context of Use (COU) in drug development. A key finding, as reflected in the program’s design, is that qualification de-risks drug development by allowing a tool to be used in any regulatory submission for its qualified COU without needing to be re-validated each time. The program is designed to foster stakeholder collaboration, encouraging the development of tools that can benefit the entire research community, thereby reducing the burden on individual sponsors.

Program Activities (Recommendations)
The structure of the DDT programs serves as a series of recommendations for tool developers:
Engage Early and Collaboratively: The programs are designed to provide a framework for early and ongoing scientific collaboration with the FDA to facilitate the development of new tools.
Follow a Staged Process: Developers are guided through a multi-stage process, typically involving a Letter of Intent, a Qualification Plan, and a Full Qualification Package, to systematically build the evidence needed for qualification.
Seek Public Qualification: The ultimate recommendation is to achieve public qualification for a DDT, which makes the tool available for broad use and integrates it into the regulatory review process, expediting future drug development.

Regulatory Considerations
The DDT Qualification Programs are a formal regulatory framework established under the 21st Century Cures Act. A “qualified” DDT has a specific regulatory status; it can be relied upon to have a specific interpretation and application in drug development and regulatory review for its stated Context of Use (COU). This qualification is publicly available and allows the tool to be included in Investigational New Drug (IND), New Drug Application (NDA), or Biologics License Application (BLA) submissions without the FDA needing to reconsider its suitability. This creates a more efficient and predictable regulatory compliance pathway for sponsors who use the qualified tool.

Keywords

Biomarker development Biomarkers Clinical outcome assessment (COA) Drug development Drug development tools (DDTs) FDA FDA guidance Regulatory compliance Regulatory framework Regulatory science Sponsor experiences Stakeholder collaboration

Technologies

AI & algorithm tools Clinical decision & monitoring systems Digital biomarkers Outcome measures & COAs

Open Resource

Some summaries are generated with the help of a large language model; always view the linked primary source of a resource you are interested in.

fda spotlight

“When submitters enter the qualification process, they agree that the qualified DDT will be made publicly available for use in drug development programs in the specified COU.”

– Section VI, p 10

Qualification Process for Drug Development Tools Guidance for Industry and FDA Staff

Qualification Process for Drug Development Tools Guidance for Industry and FDA Staff

2020 FDA

FDA guidance – final

Authors

Center for Drug Evaluation and Research, Center for Biologics Evaluation and Research

This guidance outlines the qualification process for Drug Development Tools (DDTs) under Section 507 of the Federal Food, Drug, and Cosmetic Act (FD&C Act), focusing on biomarkers, clinical outcome assessments (COAs), and animal models. The document describes a three-stage qualification process (Letter of Intent, Qualification Plan, and Full Qualification Package), emphasizing the importance of defining a specific Context of Use (COU) for each DDT. It also discusses the collaborative role of biomedical consortia and promotes transparency through public disclosure of qualification-related information. Qualified DDTs are intended to facilitate regulatory decision-making and streamline drug development.

Findings
Limited awareness and clarity regarding the qualification process and evidentiary expectations.
High resource and data demands for robust qualification submissions, particularly for novel DDTs.
Challenges in integrating multidisciplinary expertise to develop and validate DDTs.
Dependence on effective collaboration among stakeholders, including academia, industry, and regulatory bodies.
Potential delays in submission reviews if deficiencies are identified during initial assessments.

Recommendations
Define a clear and scientifically robust Context of Use (COU) for each DDT to streamline the qualification process.
Engage with FDA through early meetings to align on submission expectations and address potential gaps.
Leverage biomedical consortia and partnerships to pool resources and expertise for DDT development and validation.
Provide detailed study protocols, data analyses, and evidence in submissions to support DDT reliability and applicability.
Utilize FDA’s NextGen Portal for submission tracking and ensure compliance with recommended data standards.

Regulatory Considerations
Compliance with the three-stage qualification process: Letter of Intent (LOI), Qualification Plan (QP), and Full Qualification Package (FQP).
Adherence to transparency provisions under the 21st Century Cures Act, including public disclosure of qualification information and Determination Letters.
Rescission or modification of a qualified DDT or COU if new evidence challenges its validity.
Clear distinction between qualification for regulatory decision-making and approval for clinical use or marketing.
Encouragement to use study data standards (e.g., Clinical Data Interchange Standards Consortium) for submissions to ensure consistency and quality.

Keywords

Biomarkers Clinical outcome assessment (COA) Context of use (COU) Drug development Drug development tools (DDTs) FDA guidance Regulatory framework Regulatory science Stakeholder collaboration Validation

Technologies

Digital assessments & cognitive tools Digital biomarkers

Open Resource

Some summaries are generated with the help of a large language model; always view the linked primary source of a resource you are interested in.

The DDT Qualification process

The process involves three main stages:

Timeline: The full process typically spans several years. FDA provides feedback at each stage, but qualification is not guaranteed; evidence must meet a high bar.

COA vs. Biomarker: Which Pathway?

For sDHT-derived measures in drug development, the classification of your measure affects the evidentiary expectations and qualification pathway:

Note: This classification should be established early (see Section 2.2: Context of Use) and confirmed through regulatory engagement before committing to a qualification pathway. Misclassification can result in pursuing the wrong evidentiary strategy.

ISTAND Pilot program

The Innovative Science and Technology Approaches for New Drugs (ISTAND) Pilot Program offers an alternative pathway for novel methodologies, including sDHT-derived measures, that don’t fit neatly into existing DDT categories.

What ISTAND offers:

• Early feedback on novel approaches that may not yet meet the evidentiary bar for full qualification

• Opportunity to demonstrate proof-of-concept for innovative measures

• A “fit-for-purpose” conclusion that, while not full qualification, indicates regulatory acceptance for specific applications

When to consider ISTAND:

• Your measure is truly novel and doesn’t have clear precedent

• You want regulatory feedback on an innovative methodology before investing in full qualification

• You’re exploring approaches that could eventually support DDT qualification but aren’t ready yet

“The Innovative Science and Technology Approaches for New Drugs (ISTAND) Program accepts submissions for qualification of types of drug development tools (DDTs) that are out of scope for existing DDT qualification programs but may still be beneficial for drug development.”

– FDA, 2025

What it takes to qualify a digital endpoint

In 2023, the European Medicines Agency (EMA) qualified stride velocity 95th centile (SV95C)—a measure derived from wearable sensors—as an acceptable secondary endpoint in Duchenne muscular dystrophy trials.

While this example comes from EMA rather than FDA, it illustrates the type of multi-stakeholder effort and evidentiary package that can support qualification of an sDHT-derived measure.

Example: Stride Velocity 95th Centile (SV95C) in Duchenne Muscular Dystrophy

Key elements of the qualification:

Addressed a clear unmet need: existing endpoints (like the 6-minute walk test) were inadequate for the patient population

Built on years of collaborative work across industry, academia, and patient groups

Demonstrated that the measure captures meaningful aspects of patient function in daily life

Provided robust validation evidence across multiple studies

Qualification Opinion for Stride velocity 95th centile as primary endpoint in studies in ambulatory Duchenne Muscular Dystrophy studies

Qualification Opinion for Stride velocity 95th centile as primary endpoint in studies in ambulatory Duchenne Muscular Dystrophy studies

2023 EMA

Qualification opinion

Authors

European Medicines Agency

This document presents the qualification of stride velocity 95th centile (SV95C), measured via wearable devices, as a primary endpoint for clinical trials involving ambulant patients with Duchenne muscular dystrophy (DMD). The SV95C demonstrates strong correlation with traditional endpoints like the 6-minute walk test (6MWT) while offering advantages such as reduced bias from clinic settings, higher sensitivity to changes, and continuous real-world data collection. Validation includes qualitative and quantitative analyses, showing reliability, accuracy, and responsiveness to disease progression and treatment effects.

Findings
SV95C provides a reliable and sensitive measure of maximal ambulation, addressing limitations of traditional assessments like the 6MWT.
Real-world data collection via wearable devices enhances accuracy and reflects true ambulatory capabilities.
Longitudinal studies confirmed SV95C’s ability to detect disease progression and response to corticosteroid treatments.
Correlations with existing clinical outcome assessments (6MWT, NSAA, and 4SC) validate SV95C’s construct validity.
Patients and caregivers support the use of wearable devices in clinical trials, emphasizing reduced burden and improved trial attractiveness.

Recommendations
Use SV95C as a primary endpoint in DMD clinical trials to monitor maximal stride velocity in real-world conditions.
Incorporate SV95C alongside traditional endpoints to ensure comprehensive assessment of therapeutic efficacy.
Establish training protocols for patients and caregivers to optimize compliance with device usage.
Expand normative data for SV95C in younger and more diverse patient populations.
Conduct further research on meaningful change thresholds (MCTs) to refine clinical relevance.

Regulatory Considerations
Ensure SV95C is included as a primary endpoint with supporting secondary endpoints (e.g., muscle strength assessments) for consistency.
Validate wearable devices used for SV95C measurement to meet regulatory standards for accuracy and reliability.
Address variability and standardize protocols for data collection to ensure regulatory compliance.
Collect additional longitudinal data to strengthen the predictive value of SV95C for regulatory submissions.
Incorporate privacy and data security measures to comply with data protection regulations, including anonymization and encryption.

Keywords

Analytical validation Clinical trial endpoints Clinical trials Clinical validation Digital outcome measures Drug development tools (DDTs) EMA guidance Meaningful outcome measures Novel endpoints Pivotal trials Primary endpoint Real-world data (RWD) Sensor data integration Validation Wearables

Technologies

Clinical decision & monitoring systems Digital biomarkers Wearables & activity monitors

Open Resource

Some summaries are generated with the help of a large language model; always view the linked primary source of a resource you are interested in.

key takeaways

Regardless of whether you’re working in a medical device or drug/biologic context, several principles apply:

1. Qualification is optional and resource-intensive, but can yield significant value for future use.
It may be the right path when you’re building a tool for broad, multi-program use, not single-program applications.

2. Know which pathway applies.
MDDT qualification supports medical device submissions (CDRH). DDT qualification supports drug and biologic submissions (CDER/CBER).

3. Classification matters.
For DDT qualification, determine early whether your measure is a COA or biomarker, as this shapes your evidentiary strategy and the specific program you’ll pursue.

4. Engage FDA early in the qualification journey.
Use Pre-Submissions (for MDDT) or the Letter of Intent stage (for DDT) to confirm your approach.

5. Consider precompetitive collaboration.
Qualification is often more feasible when costs and evidence generation are shared across adopters, developers, patient groups, and academic partners.