ACPS Meeting, October 19-20, 2004 BioINequivalence: Concept and Definition Lawrence X. Yu, Ph. D. Director for Science Office of Generic Drugs, OPS, CDER,

Slides:

Advertisements

Similar presentations

Equivalence Tests in Clinical Trials

Advertisements

Dale P. Conner, Pharm.D. Division of Bioequivalence

Development of Evaluation and Consultation on Bridging Studies: Thailand Experiences Suchart Chongprasert, Ph.D. Investigational New Drug Subdivision Food.

Bioequivalence Studies Anoop Agarwal

Topical Bioequivalence Update Robert Lionberger, Ph.D. Office of Generic Drugs.

Quality by Design for Topical Dosage Forms

1 Endogenous Substance Bioavailability and Bioequivalence: Levothyroxine Sodium Tablets Steven B. Johnson, Pharm.D. Division of Pharmaceutical Evaluation.

Kyiv, TRAINING WORKSHOP ON PHARMACEUTICAL QUALITY, GOOD MANUFACTURING PRACTICE & BIOEQUIVALENCE Statistical Considerations for Bioequivalence.

Bioequivalence of Highly Variable (HV) Drugs: Clinical Implications Why HV Drugs are Safer Leslie Z. Benet, Ph.D. Professor of Biopharmaceutical Sciences.

Evaluation of quality and interchangeability of medicinal products - EAC/EC/WHO Training workshop / September |1 | Prequalification programme:

Liposome Drug Products: Bioavailability and Bioequivalence Issues Kofi A. Kumi, R.Ph., Ph.D. Office of Clinical Pharmacology and Biopharmaceutics Division.

Kyiv, TRAINING WORKSHOP ON PHARMACEUTICAL QUALITY, GOOD MANUFACTURING PRACTICE & BIOEQUIVALENCE Introduction to the Discussion of Bioequivalence.

What is a Generic Medication?. The World Health Organization Definition of a Generic Medication A generic drug is a pharmaceutical product, usually intended.

The ICH E5 Question and Answer Document Status and Content Robert T. O’Neill, Ph.D. Director, Office of Biostatistics, CDER, FDA Presented at the 4th Kitasato-Harvard.

Development and Review Process of NDA, ANDA/AADA and OTC Dr. Basavaraj K. Nanjwade M. Pharm., Ph. D Associate Professor Department of Pharmaceutics KLE.

Dale P. Conner, Pharm.D. Division of Bioequivalence OGD, CDER, FDA

Bioavailability and Bioequivalence

Clinical Pharmacology Overview From the Antiviral Perspective Kellie Schoolar Reynolds, Pharm.D. Pharmacokinetics Team Leader Office of Clinical Pharmacology.

Hanoi, WORKSHOP ON PREQUALIFICATION OF ARV: BIOEQUIVALENCE Introduction to the Discussion of Bioequivalence Study Design and Conduct Presented.

Artemisinin combined medicines, Kampala, February |1 | Training workshop on regulatory requirements for registration of Artemisinin based combined.

WHO Prequalification Program Workshop, Kiev, Ukraine, June 25-27,2007.

Individual Bioequivalence Lawrence J. Lesko, Ph.D. Director Office of Clinical Pharmacology and Biopharmaceutics Advisory Committee for Pharmaceutical.

Interchangeability and study design Drs. Jan Welink Training workshop: Training of BE assessors, Kiev, October 2009.

FDA Nasal BA/BE Guidance Overview

Qian H. Li, Lawrence Yu, Donald Schuirmann, Stella Machado, Yi Tsong

Bioequivalence of Topical Drug Products

Documentation of bioequivalence Drs. J. Welink Workshop on WHO prequalification requirements for reproductive health medicines, Jakarta, October 2009.

Bioequivalence Studies Dr Sanet Aspinall, PhD Managing Director AddClin Research Pretoria 20 March 2009.

1 Process to Address Specifications for Delivered Dose Uniformity of Inhaled and Nasal Drug Products Presented by Robert O’Neill, Ph.D. Chair ACPS Working.

Dermatopharmacokinetics Perspectives from Bioequivalence Viewpoint Historical Development of Dermatopharmacokinetics and Overview of the Guidance Vinod.

Ajaz S. Hussain, Ph.D. Deputy Director Office of Pharmaceutical Science, CDER, FDA ACPS Subcommittee on Manufacturing Science: Identification and Prioritization.

1 Bioequivalence of Highly Variable Drugs: Regulatory Perspectives Sam H. Haidar, R.Ph., Ph.D. Pharmacometrics Office of Generic Drugs.

Week 6- Bioavailability and Bioequivalence

Regulatory requirements Drs. Jan Welink Training workshop: Assessment of Interchangeable Multisource Medicines, Kenya, August 2009.

1 Axcan Public Presentation for the FDA Pharmaceutical Science and Clinical Pharmacology Advisory Committee Meeting July 23, 2008.

Highly Variable Drugs – Bioequivalence Issues: FDA Proposal Under Consideration Barbara M. Davit, J.D., Ph.D. Deputy Director, Division of Bioequivalence.

SYSTEMIC ABSORPTION AS THE MOST ACCURATE AND SENSITIVE METHOD OF DETERMINING BIOEQUIVALENCE OF GENERIC TOPICAL PRODUCTS Chris Hendy Ph.D. Novum Pharmaceutical.

Issues in Generic Substitution: Safety/Efficacy, Cost Savings and Supply Robert J. Herman, MD, FRCPC Professor, Department of Medicine University of Calgary.

Evaluation of quality and interchangeability of medicinal products - WHO Training workshop / 5-9 November |1 | Prequalification programme: Priority.

AXINN, VELTROP & HARKRIDER LLP © 2007 | AXINN, VELTROP & HARKRIDER LLP Click To Modify Title Name Goes Here Bioequivalence - What Patent.

Statistical considerations Drs. Jan Welink Training workshop: Assessment of Interchangeable Multisource Medicines, Kenya, August 2009.

WHO Workshop on Prequalification of Medicines Programme, Abu Dhabi, October, 2010 Regulatory principles reflected in practice of WHO PQP Milan Smid,

Center for Professional Advancement Generic Drug Approvals Course Bioequivalence & Bioavailability Michael A. Swit, Esq. Vice President.

Bioequivalence of Locally Acting Gastrointestinal Drugs: An Overview

CHEE 4401 Definitions drug - any substance that affects the structure or functioning of an organism pharmaceutics - the area of study concerned with the.

Bioequivalence Dr Mohammad Issa Saleh.

WHO Prequalification Programme June 2007 Training Workshop on Dissolution, Pharmaceutical Product Interchangeability and Biopharmaceutical Classification.

Bioavailability Dr. Basavaraj K. Nanjwade M. Pharm., Ph. D Department of Pharmaceutics Faculty of Pharmacy Omer Al-Mukhtar University Tobruk, Libya.

Dermatopharmacokinetics (DPK)

Pre-qualification Program: Priority Medicines Interchangeability of Multi Source Drug Products SALOMON STAVCHANSKY, PH.D. ALCON CENTENNIAL PROFESSOR OF.

Using Product Development Information to Address the Bioequivalence Challenges of Highly-variable Drugs Lawrence X. Yu, Ph. D. Director for Science Office.

Introduction What is a Biowaiver?

Malaysia, EVALUTION OF DOSSIERS IN WHO- PREQUALIFICATION PROJECT MULTISOURCE TB-DRUGS Evaluation of bioavailability/bioequivalence data Based,

Bioavailability and Bioequivalence L 10,11.  Bioavailability is a measurement of the rate and extent (amount) to which the active ingredient or active.

Exact PK Equivalence for a bridging study Steven Novick, Harry Yang (MedImmune) and Xiang Zhang (NC State) NCB, October 2015.

Bioequivalence Criteria Research Plan Stella G. Machado, Ph.D. Office of Biostatistics and the Replicate Design Technical Committee Advisory Committee.

Lawrence X. Yu, Ph.D. Director for Science Office of Generic Drugs, OPS, CDER, FDA ACPS Meeting, ACPS Meeting, Oct. 22, 2003 Office of Generic Drugs Research.

Individual Bioequivalence: Have the Opinions of the Scientific Community Changed? Leslie Z. Benet, Ph.D. University of California San Francisco.

Evaluation of quality and interchangeability of medicinal products - WHO Training workshop / 5-9 November |1 | Prequalification programme: Priority.

Federal Institute for Drugs and Medical Devices The BfArM is a Federal Institute within the portfolio of the Federal Ministry of Health 1 Statistical Considerations.

Interchangeability and study design Drs. Jan Welink Training workshop: Assessment of Interchangeable Multisource Medicines, Kenya, August 2009.

FDA Advisory Committee for Pharmaceutical Science and Clinical Pharmacology July 22-23, 2008 Introduction and Update Helen N. Winkle Director, Office of.

Topic #2: Quality by Design and Pharmaceutical Equivalence Ajaz S. Hussain, Ph.D. Office of Pharmaceutical Science Center for Drug Evaluation and Research.

SOME ISSUES ON THE DETERMINATION OF BIOEQUIVALENCE FOR HIGHLY VARIABLE DRUGS Laszlo Endrenyi University of Toronto Laszlo Tothfalusi Semmelweis University.

Ajaz S. Hussain, Ph.D. Office of Pharmaceutical Sciences CDER, FDA October 21, 2003 Dose Content Uniformity: Parametric Tolerance Interval Approach.

In vitro - In vivo Correlation

Chapter 8 BIOAVAILABILITY & BIOEQUIVALENCE

Applications of Pharmacokinetics

Suzanne M. Sensabaugh, MS, MBA

Bioequivalence trials: design, evaluation, regulatory requirements

Presentation transcript:

ACPS Meeting, October 19-20, 2004 BioINequivalence: Concept and Definition Lawrence X. Yu, Ph. D. Director for Science Office of Generic Drugs, OPS, CDER, FDA Lawrence X. Yu, Ph. D. Director for Science Office of Generic Drugs, OPS, CDER, FDA

2 Bioavailability: Rate and Extent of Drug Absorption ln Concentration AUC Time C max Time Concentration T max - time of maximum concentration

3 Bioequivalence “ the absence of a significant difference in the rate and extent to which the active ingredient or active moiety in pharmaceutical equivalents or pharmaceutical alternatives becomes available at the site of drug action when administrated at the same molar dose under similar conditions in an appropriately designed study…” (21 CFR §320.1) “ the absence of a significant difference in the rate and extent to which the active ingredient or active moiety in pharmaceutical equivalents or pharmaceutical alternatives becomes available at the site of drug action when administrated at the same molar dose under similar conditions in an appropriately designed study…” (21 CFR §320.1)

4 Bioequivalence l 90% confidence interval for AUC and Cmax between % l Passing (among others) allows market access u Generic: ANDA approval u Innovator: Demonstrates to be marketed formulation is equivalent to clinical formulation l 90% confidence interval for AUC and Cmax between % l Passing (among others) allows market access u Generic: ANDA approval u Innovator: Demonstrates to be marketed formulation is equivalent to clinical formulation

5 Why define BioINequivalence? l FDA receives studies that attempt to reverse a previous finding of bioequivalence. u Need standard to evaluate the claim l Published claims of BioINequivalence l FDA receives studies that attempt to reverse a previous finding of bioequivalence. u Need standard to evaluate the claim l Published claims of BioINequivalence

6 What Should Bioinequivalence Mean? l Bioequivalence leads to market access u A study that demonstrates bioequivalence is clear and convincing evidence of equivalence l Bioinequivalence may lead to market exclusion u A study that demonstrates bioinequivalence is clear and convincing evidence of a problem l Bioequivalence leads to market access u A study that demonstrates bioequivalence is clear and convincing evidence of equivalence l Bioinequivalence may lead to market exclusion u A study that demonstrates bioinequivalence is clear and convincing evidence of a problem

7 Possible Outcome of BE Studies T/R (%) 80%125% Demonstrate BE Fail to Demonstrate BE Fail to Demonstrate BIE Demonstrate BIE

8 Fail to Demonstrate vs. Demonstrate T/R (%) 80%125% Demonstrate BIE ? Demonstrate BE

9 Objective l To develop bioinequivalence criteria that are u Scientifically sound u Statistically valid u Fair to all parties u Easy to use l To develop bioinequivalence criteria that are u Scientifically sound u Statistically valid u Fair to all parties u Easy to use

10 April 14, 2004 ACPS Meeting l Does the ACPS agree with the distinction between demonstrating bioINequivalence and failure to demonstrate bioequivalence? u Committee’s comments: The Committee felt that there was a need to establish criteria for bioINequivalence evaluation and the criteria should not be just as failure of the bioequivalence test. The members argued it was important to focus on the clinical relevance with the therapeutic index. The Committee discussed both Area under the Curve (AUC) and Cmax as metrics important for bioequivalence and bioINequivalence. l Does the ACPS agree with the distinction between demonstrating bioINequivalence and failure to demonstrate bioequivalence? u Committee’s comments: The Committee felt that there was a need to establish criteria for bioINequivalence evaluation and the criteria should not be just as failure of the bioequivalence test. The members argued it was important to focus on the clinical relevance with the therapeutic index. The Committee discussed both Area under the Curve (AUC) and Cmax as metrics important for bioequivalence and bioINequivalence.

11 April 14, 2004 ACPS Meeting l Does the ACPS recommend a preferred method for evaluating the three pharmacokinetic endpoints for bioINequivalence? u If bioINequivalence is demonstrated for any one pharmacokinetic endpoint, then bioINequivalence is demonstrated for the products. u BioINequivalence must be demonstrated for all three pharmacokinetic endpoints for bioINequivalence to be demonstrated for the products. u There should be one pre-selected pharmacokinetic endpoint used for bioINequivalence testing. If so, which one? u The three pharmacokinetic endpoints should be evaluated for bioINequivalence with statistical corrections to the level of significance for each endpoint in order to maintain an overall significance level of l Does the ACPS recommend a preferred method for evaluating the three pharmacokinetic endpoints for bioINequivalence? u If bioINequivalence is demonstrated for any one pharmacokinetic endpoint, then bioINequivalence is demonstrated for the products. u BioINequivalence must be demonstrated for all three pharmacokinetic endpoints for bioINequivalence to be demonstrated for the products. u There should be one pre-selected pharmacokinetic endpoint used for bioINequivalence testing. If so, which one? u The three pharmacokinetic endpoints should be evaluated for bioINequivalence with statistical corrections to the level of significance for each endpoint in order to maintain an overall significance level of 0.05.

12 April 14, 2004 ACPS Meeting l Committee’s comments: u The Committee agreed on a general understanding of bioINequivalence to move forward by recognizing it is not a simple matter. In addition, the members felt this is an important concept, especially how it applies to the entire regulatory scenario. There was no consensus at this point as to a final criteria pertaining to the three pharmacokinetic endpoints. l Committee’s comments: u The Committee agreed on a general understanding of bioINequivalence to move forward by recognizing it is not a simple matter. In addition, the members felt this is an important concept, especially how it applies to the entire regulatory scenario. There was no consensus at this point as to a final criteria pertaining to the three pharmacokinetic endpoints.