FDA Regulation of Diagnostic Tests Jeffrey N. Gibbs Hyman, Phelps & McNamara, P.C. Washington, DC

Similar documents
February 2, Dear Dr. Shuren,

Primer: Medical Device User Fee Amendments Han Zhong l September 2011

Overview of the Legal Framework for Medical Device Regulation in the United States

In Vitro Diagnostic Testing for Direct Oral Anticoagulants- Premarket Review

Strengthening the Center for Devices and Radiological Health s 510(k) Review Process February 18, 2010

Preparing a US FDA Medical Device 510(K) Submission

CDRH: 510(k)S AND SCIENCE IN REGULATOR DECISION-MAKING. lannery, Scott Danzis and Christopher Pruitt. November 2010 SPECIAL REPRINT

The Path to U.S. Market for Functional Food Ingredients

Overhauling The 510(k) Process

September 28, Division of Dockets Management (HFA-305) Food and Drug Administration 5630 Fishers Lane, Room 1061 Rockville, MD 20852

FDA Oversight of Nanotechnology Applications in Foods, Food Packaging, and Nutrient Delivery

The Tobacco Control Act s Premarket Review Authorities: Reports on Substantial Equivalence and Exemption Requests (905(j))

BEST PRACTICE CHANGE CONTROL : DECIDING WHEN TO SUBMIT A 510(K) FOR A DEVICE CHANGE. Yuan Xu 18- JAN- 2018

Mitch Zeller, Director, Center for Tobacco Products, FDA September 19, 2013 Kansas Public Health Association

Key CDRH Regulatory Initiatives

Microbiology Devices; Reclassification of Influenza Virus Antigen Detection Test Systems

Industry s Perspective on the Status of Medical Device Regulations. FUNDISA Workshop 09 & 10 Oct Anele Vutha SAMED Regulatory Committee

Mark M. Yacura. Partner

Consistent with Labeling Final Guidance: Implications for Devices

May 7, Dear Mr. Landa:

Introduction. Current status of 510(k) clinical data requirements. 1 Current Status&Considerations:

FDA 510(k) 101 The Basics


510(k) submissions. Getting US FDA clearance for your device: Improving

NDI: LOOKING BACK & AHEAD

December 4, 2017 VIA ELECTRONIC SUBMISSION

Manufacturer Sponsored Speech

FDA s 510(k) Working Group

Vision and strategies to Increase Access to Innovative HIV Diagnostic Technologies. Willy Urassa. AMD STAKE HOLDERS MEETING 7-8 May 2013

Generic Drug User Fee Amendments of 2012; Regulatory Science Initiatives; Public Hearing;

Medical Device Regulatory Decision Points

Class II Special Controls Guidance Document: Intraoral Devices for Snoring and/or Obstructive Sleep Apnea; Guidance for Industry and FDA

Medical Devices and the Public s Health: The FDA 510(k) Clearance Process at 35 Years. Written Statement of

tens_(transcutaneous_electrical_nerve_stimulator) 7/ / / /2014 This policy is NOT effective until January 13, 2015

Use of Standards in Substantial Equivalence Determinations

ANDA Arthur P. Bedrosian, President Armenpharm, Ltd. 49 South Ridge Road P.O. Box D1400 Pomona, NY December 3, 2015

TOBACCO PRODUCT OR MEDICAL PRODUCT?

Draft Guidance for Industry and FDA Staff

Guidance for Industry DRAFT GUIDANCE. This guidance document is being distributed for comment purposes only.

FDLI s Enforcement, Litigation, and Compliance Conference. Center for Tobacco Products Office of Compliance and Enforcement 2017 Update

MEETING THE STANDARDS: FDA MANDATORY RAPID INFLUENZA DETECTION TEST (RIDTs) RECLASSIFICATION

The Marketing of a Food Ingredient Understanding a System that has Worked for 105 Years

FDA issues final guidance on benefit-risk factors to consider in medical device product availability, compliance, and enforcement decisions

The New Regulations - Special IVD Issues

Philip Morris USA Inc. v. FDA

Status Update on the Review of DMFs

Tobacco Product Applications: FDA Perspective

Genetically Modified Organism (GMO) Legislation and Litigation: Challenges and Opportunities

Submission to the Senate Community Affairs Legislation Committee inquiry into the Therapeutic Goods Amendment (2016 Measures No.

May 16, Division of Dockets Management (HFA-305) Food and Drug Administration 5630 Fishers Lane, Room 1061 Rockville, MD 20852

ACTION: Notification; declaratory order; extension of compliance date.

College of American Pathologists

General Wellness: Policy for Low Risk Devices Guidance for Industry and Food and Drug Administration Staff

NEURONETICS. 510(k) SUMMARY NEUROSTAR TMS THERAPY SYSTEM'

PIC/S GUIDANCE ON CLASSIFICATION OF GMP DEFICIENCIES

Taylor C. Wallace, PhD, CFS, FACN, March 22, 2018

February 15, AtriCure, Inc. Melissa Smallwood Regulatory Affairs Specialist 7555 Innovation Way Mason, Ohio 45040

Corporate Medical Policy

Overview of Regulatory Science of Food Contact Substances

FDA Foods Program Update

FDA Warning Letters Study

RESEARCH INVOLVING PRISONERS

In Vitro Diagnostic Glucose Test System

January 7, Dear Ms. Chung:

Putting the Nutritional Supplement Industry to the Test: Looking for Transparency

Guidance - IDE Early/Expanded Access for Devices

The proposed rule is significant, and the requirements and exceptions are complex. Key provisions of the proposal are described below.

Laboratory Developed Tests (LDTs) and the FDA: The Impact on Clinical Laboratories

Regulatory Framework for Medical Devices in South Africa. 23 November 2018 Andrea Keyter Deputy Director: Medical Devices

The Nutrition (Amendment) (EU Exit) Regulations 2018

Using Recall Data to Assess the 510(k) Process

Planning For The FDA s 'Deeming Rule' For E- Cigarettes

Introduction to Product Regulation Under the Family Smoking Prevention & Tobacco Control Act

FDA s Action Agenda to Reduce Tobacco Related-Cancer Incidence and Mortality

NOV Jo 6) ' 510(k) Summary

Political Economy of the Medical Products Industry

Update on WHO Prequalification of In Vitro Diagnostics

Re: Docket No. FDA D Presenting Risk Information in Prescription Drug and Medical Device Promotion

U.S. Department of Health and Human Services Food and Drug Administration Center for Devices and Radiological Health. Preface

perpetuate -- and perhaps even intensify -- that controversy. 1 On July 18th, the Fifth Circuit affirmed FDA s longstanding position that

Our medtech experts are yours. 510(k)s for Connected Medical Devices.

REGULATORY CHALLENGES IN SOUTH AFRICA

International Pharmaceutical Aerosol Consortium on Regulation and Science

February 15, AtriCure, Inc. Melissa Smallwood Regulatory Affairs Specialist 7555 Innovation Way Mason, Ohio 45040

IRB review of device studies

Regulatory Update: Food Safety and Nutrition

IRB Policy 5 Research Activities

THE US FDA S CUSTOM DEVICE EXEMPTION Practical Solutions for Handling the Sale of Patient-Specific Devices in the USA. August 2011 SPECIAL REPRINT

GLP Update and Hot Topics

Premarket Review. FFDCA Section 201(s) FFDCA Section 201(s) (cont.)

Food Additives Program

2/17/2018. Prof. Steven S. Saliterman Department of Biomedical Engineering, University of Minnesota

Prof. Steven S. Saliterman. Department of Biomedical Engineering, University of Minnesota

2014 FDA/JIFSAN Food & Nutrition Webinar

Global Regulation of Food Additives

DETERMINING WHETHER AN ACTIVITY IS HUMAN SUBJECTS RESEARCH AS DEFINED BY FEDERAL REGULATIONS

Guide to Interchangeable Medicines

,,~ 30! Premarket Notification - SomnoMed MAS Flex "S"

SAMED Position: Reuse of SUDs

Transcription:

AIPLA Annual Meeting Joint Biotechnology Committee/ Special Committee on FDA Law Program October 21, 2010 Marriott Wardman Park Hotel Washington, DC FDA Regulation of Diagnostic Tests Jeffrey N. Gibbs Hyman, Phelps & McNamara, P.C. Washington, DC jgibbs@hpm.com

Introduction In Vitro Diagnostics (IVDs) are playing an increasingly important role in medicine. Many new types of diagnostics being developed. Introducing new diagnostics to the market presents potential regulatory challenges. 2

Definition of an IVD A product intended to be used to diagnose a disease or other condition is regulated as a device. Diagnose has been given a broad interpretation by the courts. Diagnose also encompasses screening, monitoring, prognosis, etc. Technology does not determine whether product is regulated as a device. Not all tests are diagnostic, e.g., genealogy, ancestry, etc. 3

Intended Use: A Pivotal Concept Intended Use is governed by the objective intent of the company 21 C.F.R. 801.4. Intended use can determine whether Premarket Approval (PMA), 510(k) Premarket notification, or no FDA review. Intended use can determine how much data and what type, e.g., prospective large scale study for screening study vs. small retrospective study for monitoring. Affects reimbursement. Relationship to IP? 4

Intended Use: A Pivotal Concept (cont d.) Needs to be considered at an early stage and integrated with regulatory, clinical and marketing input. Needs to match clinical data and study population. Controls claims for IVD once cleared/approved. Subtle differences can have a large regulatory impact, e.g., rule out vs. rule in. 5

Intended Use: A Pivotal Concept (cont d.) Intended use can include population tested, purpose of test, etc. An intended use is more specific than A test for Cancer X. Closely related term is indications for use. Subject to intensive negotiations with FDA. What companies end up with can be very different from their starting point. To sum up: Can determine whether PMA or 510(k), what data need to be collected (time and cost), reimbursement coverage, and marketing strategy. 6

In Vitro Diagnostics (IVDs): Routes to the Market Premarket Approval Application 510(k) premarket notification De Novo Reclassification Investigational Use Only Research Use Only Analyte Specific Reagents Laboratory Developed Tests 7

FDA Classification Scheme Level of regulation linked to product risk. Class I low risk. 510(k) generally not needed; may be exempt from Good Manufacturing Practice (GMP) regulation. Example: Equine encephalomyelitis virus serological reagents. Class II moderate risk. Usually subject to 510(k) and GMP. Example: Glucose. May also need to meet special controls. Class III highest risk. PMA required. Example: Human Papilloma Virus assays and cancer screening tests. Risk is independent of performance of the assay. 8

510(k) Premarket Notification Most common route to market with new assay. Need to show substantial equivalence to a predicate device. Predicate devices on the market before May 28, 1976 or cleared by FDA through a 510(k). PMA approved device cannot be a predicate device for a 510(k), unless reclassified. 9

510(k) Premarket Notification (cont d.) Substantial equivalence. Same intended use, though FDA has some flexibility in applying requirement. Same technology, or technological differences do not raise different issues of safety or effectiveness. Typically, the use of novel technology, such as proteinbased markers, does not preclude 510(k) clearance. Will need to provide performance data. The kinds of data requested may be affected by type of technology and its novelty. Clinical data will be required for new types of assay. Analytical test data, e.g., reproducibility, will be required. 10

510(k) Premarket Notification (cont d.) FDA can find Substantially Equivalent, allowing IVD to be marketed. Can find 510(k) Not Substantially Equivalent, i.e., reject it. Ask for more information. 90 days per review cycle. Recently, many criticisms of 510(k) process. FDA has unveiled internal reports on the 510(k) process, with many recommendations. In general, will make 510(k)s more challenging. 11

De Novo Classification Some low or moderate risk devices lack predicate device. For these products, FDA can use de novo classification process. Company submits 510(k). Found Not Substantially Equivalent. Then submit petition for de novo classification. FDA can then clear the device. FDA will issue special controls guidance document. 12

De Novo Classification (cont d.) FDA has used de novo process about two times per year for IVDs, e.g., circulating tumor cells for breast cancer, and recent ovarian cancer test. FDA prefers to use 510(k) if possible because less work, since no guidance document needed. Subsequent applicants can use 510(k) process. 13

Premarket Approval Application Requires clinical data. Voluminous submission. 180 day review cycle. Advisory panel for at least the first submission for that type of assay. Pre-approval GMP inspection. FDA typically monitors study sites. More costly than 510(k)s and generally takes longer. Once obtain approval, harder to make changes. 510(k) route is preferred. Potential exclusivity impact of IVD intended to be used diagnostically with drug? Can get patent term extension. 14

Investigational Use Only (IUO) IUO products are intended for use in clinical investigations. Vehicle for generating clinical data to support marketing application. Can charge for IUO products within limits. Product must be labeled as IUO. Sponsor needs to receive some data back from investigators. Limited promotional claims. Manufacturer can sell IUO products. Clinical trial agreement between sponsor and investigator. Should include IP-related clauses IUO products may have protection from patent infringement claims. 15

Investigational Use Only (IUO) (cont d.) Generally, FDA approval not needed to begin study. Typically will need approval from an institutional review board for prospective studies, and possibly for retrospective. May need to obtain patient informed consent. Banked specimens can be used under some circumstances. Exempt from GMP regulation. 16

Research Use Only (RUO) RUO products are intended for use in basic research or to identify a potential clinical application. Cannot claim safe, effective, or has diagnostic utility. Can charge for RUO products. No need to collect data. Exempt from GMPs. Can create reimbursement issues for laboratories. Useful for niche products, but not a successful longterm strategy for products with diagnostic value. FDA has been concerned about misuse of RUO category, and plans to issue a new draft guidance document aimed at RUO manufacturers. 17

Analyte Specific Reagents (ASRs) ASRs are building blocks for assays developed by laboratories. They are generally exempt from 510(k) or PMA, but do need to comply with GMPs. In a guidance document issued in September 2007, FDA substantially narrowed the scope of ASRs. Can contain only a single marker, e.g., no primer/pair probes. Cannot be on a bead or something similar. 18

Laboratory Developed Tests (LDTs) LDTs are subject to the Clinical Laboratory Improvement Amendment. FDA first said it could regulate LDTs in 1992. According to FDA, all LDTs are medical devices and subject to full device regulation. FDA did not seek to exercise power until a few years ago. Exercising it more frequently, e.g., Warning Letter to LabCorp regarding OvaSure. Issue: How much work does a lab need to do for a test to qualify as LDT? 19

Laboratory Developed Tests (LDTs) (cont d.) FDA has stated it intends to no longer exercise enforcement discretion over LDTs, but will actively regulate them. Two-day public meeting in July to discuss. Commenters did not oppose concept of FDA regulation. Considerable concern about manner in which regulation would occur, particularly for rare/orphan diseases and emerging diseases, and cost of regulation. FDA has said prioritization scheme will be risk-based. Diagnostics that guide drug therapy will be priority for being brought under FDA regulation. 20

Laboratory Developed Tests (LDTs) (cont d.) Will take some time for details of framework to be developed. FDA has said does not intend to disrupt current testing. Grandfather period for tests on the market. Grace period, i.e., delayed effective date. Impact on innovation? Impact on FDA workload? FDA s regulation of LDTs may prompt litigation. Begin by requiring registration of laboratories? 21

Conclusion Public health impact increasing. IVDs represent a large and growing industry. Complex, evolving regulatory environment. 22

2024 © healthdocbox.com Privacy Policy | Terms of Service | Feedback