Challenges in the Regulation of Pediatric Clinical Trials

Similar documents
First In Human Pediatric Trials and Safety Assessment for Rare and Orphan Diseases

Roles & Responsibilities of the Sponsor

February 2006 Procedural

Guidance for Industry

Guidance for Industry

4.1 Objectives of Clinical Trial Assessment

Regulatory Pathways for Licensure and Use of Ebola Virus Vaccines During the Current Outbreak FDA Perspective

Guidance for Industry FDA Approval of New Cancer Treatment Uses for Marketed Drug and Biological Products

Rare Diseases: Common Issues in Drug Development Guidance for Industry

Guidance for Industry and FDA Staff

Breakthrough Therapy Program U.S. Food and Drug Administration (FDA)

BIOTECHNOLOGY OPERATIONS

CLINICAL TRIALS SHOULD YOU PARTICIPATE? by Gwen L. Nichols, MD

Overview of Phase 1 Oncology Trials of Biologic Therapeutics

Guidance for Industry

Proof-of-Concept Studies and the End of Phase IIa Meeting with the FDA

Overview of Drug Development: the Regulatory Process

Ethical Principles in Clinical Research. Christine Grady Department of Bioethics NIH Clinical Center

Sheffield Kidney Institute. Planning a Clinical Trial

Formal FDA Meeting Request: Guidance and Template

Achieving Regulatory Success: Areas of focus for biotechnology companies. Michael J. Schlosser, PhD, DABT April 21, 2013

Expanded Access Programs. Richard Klein Office of Special Health issues Food and Drug Administration

Guidance for Industry

Biosimilars: Additional Questions and Answers Regarding Implementation of the Biologics Price Competition and Innovation Act of 2009

Guidance for Industry Investigator Responsibilities Protecting the Rights, Safety, and Welfare of Study Subjects

Guidance for Industry and Investigators Safety Reporting Requirements for INDs and BA/BE Studies- Small Entity Compliance Guide

FAST TRACK DEVELOPMENT OF EBOLA VACCINES: FDA REGULATORY PERSPECTIVE

Ethical Issues Surrounding the Conduct of Pediatric Clinical Studies

Guidance for Industry Expedited Programs for Serious Conditions Drugs and Biologics

Special Considerations for Pediatric Trials

Best Practices in Clinical Research Protocol Writing: Eight tips from an IRB member

Guidance for Industry

University of Hawai i Human Studies Program. Guidelines for Developing a Clinical Research Protocol

Guidance for Industry and FDA Staff FDA Acceptance of Foreign Clinical Studies Not Conducted Under an IND Frequently Asked Questions

Guidance for Industry

Principal Investigator and Sub Investigator Responsibilities

Glossary of Clinical Trial Terms

Clinical Trials in Thalassemia Cell and Gene Therapy Grant Award

Guidance for Industry Independent Consultants for Biotechnology Clinical Trial Protocols

Information Sheet Guidance for Sponsors, Clinical Investigators, and IRBs

Guidance for Industry

Guidance for IRBs, Clinical Investigators, and Sponsors. Considerations When Transferring Clinical Investigation Oversight to Another IRB

NONCLINICAL EVALUATION FOR ANTICANCER PHARMACEUTICALS

The Clinical Trials Process an educated patient s guide

Guidance for Clinical Investigators, Sponsors, and IRBs

Goals & Objectives. Drug Development & the FDA Pharmacy 309. Outline. An History of Disasters. Be able to describe

Guidance for Industry

Information Sheet Guidance For IRBs, Clinical Investigators, and Sponsors

CTC Technology Readiness Levels

A FDA Perspective on Nanomedicine Current Initiatives in the US

GENERAL CONSIDERATIONS FOR CLINICAL TRIALS E8

Guidance for IRBs, Clinical Investigators, and Sponsors

Clinical Trial Design. Sponsored by Center for Cancer Research National Cancer Institute

CONDUCTING GLOBAL CLINICAL RESEARCH TRIALS:

ROLE OF THE RESEARCH COORDINATOR Study Start-up Best Practices

Safety Assessment for IND Safety Reporting Guidance for Industry

ICH M3 (R2) Guideline on Nonclinical Safety Studies for the Conduct of Human Clinical Trials and Marketing Authorization for Pharmaceuticals

12.0 Investigator Responsibilities

POLICY AND PROCEDURES OFFICE OF NEW DRUGS. Good Review Practice: Management of Breakthrough Therapy-Designated Drugs and Biologics.

Enabling Discovery, Development, and translation of treatments for Cognitive Dysfunctions in Depression: A Workshop Session IV

Non-clinical development of biologics

Guidance on IRB Continuing Review of Research

Waiver to Allow Participation in a Food and Drug Administration Advisory Committee

Good Clinical Practice 101: An Introduction

Medical Billing and Agency Formal Disputes

Guidance for Industry Determining the Extent of Safety Data Collection Needed in Late Stage Premarket and Postapproval Clinical Investigations

Guidance for Industry

Guideline for Industry

COMMITTEE FOR PROPRIETARY MEDICINAL PRODUCTS (CPMP) NOTE FOR GUIDANCE ON THE PRE-CLINICAL EVALUATION OF ANTICANCER MEDICINAL PRODUCTS

Role of the Investigational Drug Services (IDS) in the Management of Investigational Drugs

EXHIBIT COORDINATING PROVISIONS-STATE/FEDERAL LAW, ACCREDITATION STANDARDS AND GEOGRAPHIC EXCEPTIONS MARYLAND

Early Drug Discovery and Development Guidelines: For Academic Researchers, Collaborators, and Start-up Companies

FDA Fast Track and Priority Review Programs

Guidance for Industry Influenza: Developing Drugs for Treatment and/or Prophylaxis

Voluntary Genomic Data Submissions at the U.S. FDA

Guidance for Industry and Review Staff Target Product Profile A Strategic Development Process Tool

U.S. Food and Drug Administration

Guidance for Industry and FDA Staff

Subject: No. Page PROTOCOL AND CASE REPORT FORM DEVELOPMENT AND REVIEW Standard Operating Procedure

Guidance on Withdrawal of Subjects from Research: Data Retention and Other Related Issues

RESEARCH STUDY PROTOCOL. Study Title. Name of the Principal Investigator

The 505(b)(2) Drug Development Pathway:

Guidance for Industry

Not All Clinical Trials Are Created Equal Understanding the Different Phases

ICH Topic E 8 General Considerations for Clinical Trials. Step 5 NOTE FOR GUIDANCE ON GENERAL CONSIDERATIONS FOR CLINICAL TRIALS (CPMP/ICH/291/95)

exactly. The need for efficiency in developing effective new therapeutics has never been greater.

RE: Human Research Subject Protections Under Federal Wide Assurance (FWA) FWA and Multiple Project Assurance (MPA) M-1167

Current and Future Applications of Probiotic Science

Information Sheet Guidance For IRBs, Clinical Investigators, and Sponsors

Guidance for Industry Diabetes Mellitus Evaluating Cardiovascular Risk in New Antidiabetic Therapies to Treat Type 2 Diabetes

Health Products and Food Branch.

ST. MICHAEL S HOSPITAL Guidelines for Reporting Serious Adverse Events / Unanticipated Problems to the SMH Research Ethics Board (REB) July 09, 2014

Basic Overview of Preclinical Toxicology Animal Models

2.2 Roles and Responsibilities in the Conduct and Assessment of Clinical Trials

Session 6 Clinical Trial Assessment Phase I Clinical Trial

Transcription:

Challenges in the Regulation of Pediatric Clinical Trials Wilson W. Bryan, M.D. FDA / CBER / OCTGT wilson.bryan@fda.hhs.gov National Institutes of Health Recombinant DNA Advisory Committee (RAC) Meeting Rockville, Maryland September 16, 2010

Challenges in the Regulation of Pediatric Clinical Trials : Outline Therapeutic Development Objective Process Regulatory Process IND Review Clinical Hold Pediatric Studies Ethical Principles Special Protections Regulatory Challenges 2

Therapeutic Development Objective: Drugs (including biologics) that are safe and effective for a given indication Process Drug discovery Nonclinical (animal) study objectives: Toxicity, biodistribution, carcinogenicity, proof-of-principle Guide design (including dosing, population, and monitoring) of subsequent Phase 1 study Phase 1 objectives: Safety, tolerability, maximum tolerated dose (MTD), pharmacokinetics, (and activity / efficacy, if feasible) Guide dosing and monitoring in subsequent Phase 2 studies Phase 2 objectives: Determine dose, route, regimen, population, endpoints, and estimated magnitude of effect Guide design of subsequent confirmatory (Phase 3) studies Phase 3 objectives: Evidence of efficacy and safety to support a marketing application (New Drug Application (NDA) or Biologics Licensing Application (BLA)) 3

Regulatory Process Investigational New Drug application (IND) Review Team Project Manager Chemistry, Manufacturing, and Controls (CMC) Nonclinical Pharmacology / Toxicology Clinical Others (e.g., statistics, epidemiology, patient representative) Objective: FDA s primary objectives in reviewing an IND are, in all phases of the investigation, to assure the safety and rights of subjects (21 CFR 312.22(a)) Clinical Hold A clinical hold is an order issued by FDA to the sponsor to delay a proposed clinical investigation or to suspend an ongoing investigation (21 CFR 312.42 (a)). 4

Regulatory Process Clinical Hold: FDA may place a proposed or ongoing Phase 1 investigation on clinical hold if it finds that (21 CFR 312.42(b)): (i) Human subjects are or would be exposed to an unreasonable and significant risk of illness or injury; (ii) The clinical investigators named in the IND are not qualified ; (iii) The investigator brochure is misleading, erroneous, or materially incomplete; (iv) The IND does not contain sufficient information to assess the risks to subjects of the proposed studies. 5

Pediatric Studies: Ethical Principles Children are a vulnerable population because they are not able to give true informed consent. Therefore, Study adults unless it is scientifically necessary to study children. Assess whether studies in adults would be relevant, ethical, feasible, and substantially accomplish the objective(s) of the study. If study of children is scientifically necessary, consider initial study of older children, who are better able to give informed consent. Regulations provide Additional Safeguards for Children in Clinical Investigations (21 CFR 50.50 50.56; Subpart D) 6

Pediatric Studies: Subpart D 50.50: IRB duties: In addition to other responsibilities assigned to IRBs, each IRB must review clinical investigations involving children as subjects covered by this Subpart D and approve only those clinical investigations that satisfy the criteria described in 50.51, 50.52, or 50.53 7

Pediatric Studies: Subpart D 50.51 Clinical investigations not involving greater than minimal risk 50.52 Clinical investigations involving greater than minimal risk but presenting the prospect of direct benefit to individual subjects. 50.53 Clinical investigations involving greater than minimal risk and no prospect of direct benefit to individual subjects, but likely to yield generalizable knowledge about the subjects disorder or condition. The risk represents a minor increase over minimal risk. OCTGT believes that gene therapy trials generally have more than a minor increase over minimal risk. Therefore, 50.51 and 50.53 generally do not apply to gene therapy trials. 8

Pediatric Studies: Subpart D OCTGT regulates gene therapy trials in children with consideration of the principles of 21 CFR 50.52. 50.52 Clinical investigations involving greater than minimal risk but presenting the prospect of direct benefit to individual subjects... may involve children as subjects only if the IRB finds and documents that : (a) The risk is justified by the anticipated benefit to the subjects; To provide evidence of the prospect of direct benefit (or the anticipated benefit), OCTGT often asks IND sponsors to provide proof-ofconcept data from nonclinical and / or previous human studies. 9

Pediatric Studies: Subpart D 50.54 Clinical investigations not otherwise approvable that present an opportunity to understand, prevent, or alleviate a serious problem affecting the health or welfare of children. If an IRB does not believe that a clinical investigation involving children as subjects meets the requirements of 50.51, 50.52, or 50.53, the clinical investigation may proceed only if: (a) The IRB finds and documents that the clinical investigation presents a reasonable opportunity to further the understanding, prevention, or alleviation of a serious problem affecting the health or welfare of children; and (b) The Commissioner of Food and Drugs, after consultation with a panel of experts in pertinent disciplines and following opportunity for public review and comment, determines [that specific conditions are met that allow the study to proceed.] If a gene therapy study is not approvable under 50.52, OCTGT does not refer the study for consideration under 50.54. OCTGT believes that such a referral for consideration should come from outside of FDA (e.g., from 10 the IND sponsor or from an IRB).

Regulatory Challenges in Pediatric Clinical Trials : For the sponsor Minimize risks while maintaining prospect of direct benefit and acceptable risk-benefit ratio What constitutes sufficient evidence of a prospect of direct benefit (i.e., proof-of-concept (POC) data)? Should nonclinical POC studies be replicated by independent groups? What is the appropriate study population? Is there an adult population that would be sufficiently informative, with an acceptable risk-benefit ratio? How to determine the starting dose? Consider available nonclinical data (e.g., NOEL and NOAEL) and previous human experience with the product or related products. What study procedures (e.g., MRI, lumbar puncture) are acceptable? Consider the risk of the procedure, the benefit (if any) of the procedure to the subject, and the value of the resulting data (benefit of generalizable knowledge). 11

Regulatory Challenges in Pediatric Clinical Trials : For the sponsor For pediatric studies, OCTGT asks the sponsor to describe the following: how the study meets the requirements of Subpart D why the study of children is scientifically necessary 12

Regulatory Challenges in Pediatric Clinical Trials : For the FDA 1. When is it appropriate for a pediatric study to be a first-in-man study for a new experimental gene therapy? 2. If adults must be studied to provide initial evidence of safety before proceeding with a study in children, how many adults must be studied? 13

Regulatory Challenges in Pediatric Clinical Trials : For the IRB To what degree do IRBs defer assessment of the science and/or ethical/human subject protection issues to other entities (e.g., FDA, RAC)? How do IRBs determine whether early stage gene or cell transfer studies have a prospect of direct benefit? How do IRBs help investigators, participants, and their families avoid a therapeutic misconception when communicating risks and anticipated benefits? 14

Public Workshop on Cell and Gene Therapy Clinical Trials in Pediatric Population November 2, 2010 Bethesda, Maryland The goal of this workshop is to gather information from stakeholders regarding best practices related to cell and gene therapy clinical trials in pediatrics including: evaluating these novel therapeutic products prior to initiating pediatric clinical studies, identifying and minimizing risks associated with the administration of cell and gene therapy products in pediatric studies, obtaining informed consent and assent, and conducting continuing review and oversight of cell and gene therapy products in pediatric studies. 15

Public Workshop on Cell and Gene Therapy Clinical Trials in Pediatric Population November 2, 2010 Bethesda, Maryland To register, contact: Bernadette Kawaley Center for Biologics Evaluation and Research (HFM-43) Food and Drug Administration, 1401 Rockville Pike, Suite 200N, Rockville, MD 20852-1448 Phone (301) 827-2000, Fax (301) 827-3079; email: CBERTraining@fda.hhs.gov (Subject line: Pediatrics Ethics Workshop). 16

Challenges in the Regulation of Pediatric Clinical Trials Wilson W. Bryan, M.D. FDA / CBER / OCTGT wilson.bryan@fda.hhs.gov National Institutes of Health Recombinant DNA Advisory Committee (RAC) Meeting Rockville, Maryland September 16, 2010

2026 © DocPlayer.net Privacy Policy | Terms of Service | Feedback  | Do Not Sell My Personal Information