EU FDA: CMC Differences - PowerPoint PPT Presentation

1 / 35
About This Presentation
Title:

EU FDA: CMC Differences

Description:

Jarosz Regulatory Services, Inc (www.jrsweb.com) ... Use of preservatives. Type of packaging. Pack sizes. Sterilization process ... – PowerPoint PPT presentation

Number of Views:810
Avg rating:3.0/5.0
Slides: 36
Provided by: maryyj
Category:

less

Transcript and Presenter's Notes

Title: EU FDA: CMC Differences


1
EU FDA CMC Differences
  • Mary Y. Jarosz, R.Ph, RAC, FTOPRA
  • Jarosz Regulatory Services, Inc (www.jrsweb.com)
  • AAPS Chicagoland Pharmaceutical Discussion Group
    (CPDG) symposium
  • April 11, 2008, Skokie, IL

2
Objectives
  • To understand the general differences between the
    EU and the US FDA CMC CTD
  • To take home practical suggestions for
    constructing CMC Module 2.3 and Module 3

3
(No Transcript)
4
EU and FDA
  • EU multiple agencies
  • European Medicines Evaluation Agency (EMEA)
    administrative organization
  • Committee for Medicinal Products for Human Use
    (CHMP) of the EMEA scientific input
  • National Health Agencies
  • FDA one agency

5
EU and FDA
  • EU multiple registration procedures
  • Centralized
  • European Community
  • Decentralized/Mutual Recognition
  • At least 2 Member States
  • National
  • 1 Member State
  • FDA one registration procedure

6
EU and FDA
  • CTD
  • More similar than different
  • Bulk of the CMC data will be the same for both
    agencies

7
CTD Defined
  • It is a harmonized format (template) for
    presenting data in the ICH regions
  • It is not a list of data requirements for
    applications
  • Result ? differences remain

8
CTD CMC Structure
  • ICH M4Q Quality
  • EU (CPMP/ICH/2887/99)
  • FDA (M4 QA guidance June 2004)
  • 2.3 QOS Quality Overall Summary (QOS)
  • 3.2.S Drug Substance (DS)
  • 3.2.P Drug Product (DP)
  • 3.2.A Appendices
  • 3.2.R Regional
  • 3.3 Literature References

9
CTD CMC Structure
  • CTD can accommodate
  • Differences in content
  • Differences in review styles
  • Local particulars
  • Specifications
  • Package configurations

10
Differences in Content
  • ICH Q4A Pharmacopeial Harmonization
  • Harmonize compendial test chapters
  • Interchangeable in the 3 ICH regions
  • Pharmacopeial Discussion Group (PDG) ? USP, JP,
    EP (PhEur)
  • 11 General Test Chapters in ICH Q6A
  • PDG submits pharmacopeial text proposals to ICH
    Q4B Expert Working Group (EWG)

11
Differences in Content
  • ICH Q4B Evaluation Recommendation
  • Expert Working Group (ICH Q4B EWG) evaluates
    pharmacopeial text proposals from PDG and
    assesses regulatory impact
  • Dialogue between PDG and Q4B EWG
  • Q4B EWG makes conclusions and recommendations in
    the ICH regions

12
www.edqm.eu
13
Differences in Review Styles
  • EMEA is an administrative framework, and National
    Agencies are the scientific reviewers
    differences in culture and medical practices
  • FDA reviewers are within the same Agency
  • EU top down, FDA bottum up
  • EU benefit/risk of entire data, FDA more specific
    (2 adequate and well-controlled studies)
  • Same data package to both will probably not
    result in the same outcome

14
Comparison of EU and US CTD
  • Module 1 Administrative (not CTD)
  • Application Form, Labeling, DMF Letters of
    Access, Environmental Risk Assessment
  • Module 2.3 QOS
  • Key review document
  • 40-80 pages Attachments
  • EU focus (the old Expert Reports)
  • Module 3 Quality (CMC)

15
Module 2.3 QOS
  • Discussion/assessment of data
  • Opportunity for the sponsor to highlight and
    explain data
  • Impurities, justify deviations from EU/FDA
    guidelines, integrate nonclinical and clinical
  • Reviewed across disciplines ? influences
    reviewers perceptions
  • Ideally written after Module 3 completed
  • Final review in conjunction with Module 3
  • May be excerpted for public disclosure

16
Module 3 Drug Master File
  • EU Active Substance Master File
  • Commonly, European Drug Master File (EDMF)
  • CPMP/QWP/227/02/rev.1
  • Applicants Part (manufacturer MAH)
  • Restricted Part (manufacturer only)
  • Certificate of Suitability (CEP)
  • European Directorate for the Quality of Medicines
    Health Care (EDQM)

17
Module 3 Drug Master File
  • US DMF
  • Type 2 drug substance, intermediate, source
    material, drug product
  • Type 3 packaging
  • Type 4 excipient, colorant, flavor

18
EU CEP and TSE CEP
  • Certification by EDQM
  • Governed by Resolution AP-CSP(07)1 and Directives
    2001/83/EC, 2001/82/EC, 2003/63/EC
  • Manufacturers or suppliers of active substances
    or excipients
  • Any product with transmissible spongiform
    encephalopathy (TSE) risk
  • CEP
  • EDQM evaluates the suitability of the PhEur
    monograph to control the chemical purity and
    microbiological quality or
  • TSE CEP
  • Evaluates the reduction of TSE risk or
  • Both

19
Module 3 EU Focus
  • EDMF only for drug substances
  • CEP for a pharmacopeial drug substances
  • TSE CEP (or BSE/TSE documentation)
  • Process Validation Scheme
  • EU supply chain
  • Standard Terms for containers, dosage forms, and
    routes of administration

20
Module 3 FDA Focus
  • Reference to DMF(s)
  • Drug Substance container closure
  • Sterility Assurance Validation package
  • 3.2.P.3.5 Process Validation or
  • 3.2.R.1 Regional
  • Executed Batch records
  • Comparability Protocols
  • Methods Validation Package

21
3.2.S Drug Substance
  • Essentially same for EU and US
  • Unless
  • reference to DMF or CEP
  • Link documents from different development sources
    for DS and DP
  • In-house and third-parties

22
3.2.S Drug Substance
  • 3.2.S.2.1 Manufacturer
  • Establishment Registration Number for US
    applications
  • 3.2.S.2.5 Process Validation
  • Commercial scale batches for FDA
  • 3.2.S.4.1/4.2/5 Specifications/Analytical
    Procedures/Reference Standards
  • Possible differences in USP and Ph.Eur

23
3.2.S Drug Substance
  • 3.2.S.7 Stability
  • Less data on existing active substances for FDA
    (1 pilot scale, 3 months accelerated)
  • In the EU, 2 options
  • 6 months at time of submission of accelerated and
    long term data on 2 production scale batches OR
  • 6 month at time of submission of accelerated and
    long term data on 3 pilot scale batches

24
3.2.P.1 Description and Composition
  • EU Composition of colors, film coating,
    printing ink (detailed in 3.2.P.4.1)
  • US DMF reference
  • Reference to compendia
  • Diluents
  • EU separate part P for diluents composed of
    more than one component
  • FDA incorporate within 3.2.P.1

25
3.2.P.2 Pharmaceutical Development
  • Excipients (colorants)
  • Nomenclature of excipients (USP and PhEur)
  • Use of preservatives
  • Type of packaging
  • Pack sizes
  • Sterilization process

26
3.2.P Drug Product
  • 3.2.P.3 Manufacturer
  • May be different
  • 3.2.P.3.5 Process Validation
  • Results at pre-approval inspection for US
  • Protocol at submission for EU
  • 3.2.P.4 Control of Excipients
  • Specifications and TMs possible differences in
    USP and PhEur

27
3.2.P.4.5 Excipients of Human/Animal Origin
  • TSE risk emphasized in EU
  • TSE CEP

28
3.2.P.5 Control of Drug Product
  • Specifications and TMs possible differences in
    USP and PhEur
  • Release and shelf-life specs (EU)
  • Release and shelf-life specs are the same (US)
  • Skip and Parametric Release testing may be viewed
    differently

29
3.2.A Appendices
  • 3.2.A.1 Facilities and Equipment for Biotech
    products
  • 3.2.A.2 Adventitious Agents Safety Evaluation
  • non-viral and viral
  • risk assessment of potential contamination with
    adventitious agents
  • 3.2.A.3 Excipients

30
3.2.R Regional EU
  • Process Validation Scheme on commercial scale
  • Reference to Medical Device

31
3.2R Regional US (DS)
  • Executed Batch Record
  • In English
  • Method Validation Package
  • For non-USP
  • Comparability Protocols (draft guidance)

32
3.2.R Regional US (DP)
  • Executed Batch Records
  • In English
  • Including equipment, packaging records, labeling
    procedures, batch and label reconciliation
  • Information on Components
  • Comparability Protocol (draft guidance)
  • Methods Validation Package
  • For non-USP

33
Electronic CTD (eCTD)
  • EU 22 Jan 2008
  • Electronic-only submissions/eCTD
  • Centralized Procedure (EMEA/5633/2007)
  • 1 July 2008 accepted ( paper)
  • 1 Jan 2009 strongly recommended (paper an
    exception)
  • European Regulatory Network end 2009
  • FDA preferred format
  • IND, NDA, BLA, ANDA, Master Files, Annual Reports

34
eCTD
  • Templates
  • Editing of MS Word documents to repair styles
  • Generating PDF documents
  • Optical character recognition (OCR) of scanned
    PDF documents
  • Bookmarks and hyperlinks
  • Publishing software / new lingo

35
Summary
  • CTD format is the standard
  • CMC for EU and FDA is more similar than different
  • There are EU / FDA CMC differences that should be
    addressed
  • CTD can accommodate EU and FDA differences in
    content, review styles, local particulars
  • eCTD is here
Write a Comment
User Comments (0)
About PowerShow.com