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    Ich and Qsem

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    Vaishnavi Karmveer
    The document discusses the International Council for Harmonisation of Technical Requirements for Pharmaceuticals for Human Use (ICH) guidelines. It provides an overview of the regulatory bodies and research-based industries involved in different regions. It then describes the process of harmonization through various steps including consensus building, confirmation of agreement, regulatory consultation and discussion, acceptance as a harmonized guideline, and implementation. It lists several Q, S, and E series guidelines covering topics like quality, safety, and efficacy.

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    Ich and Qsem

    Uploaded by

    Vaishnavi Karmveer
    101 views31 pages
    The document discusses the International Council for Harmonisation of Technical Requirements for Pharmaceuticals for Human Use (ICH) guidelines. It provides an overview of the regulatory bodies and research-based industries involved in different regions. It then describes the process of harmonization through various steps including consensus building, confirmation of agreement, regulatory consultation and discussion, acceptance as a harmonized guideline, and implementation. It lists several Q, S, and E series guidelines covering topics like quality, safety, and efficacy.

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    The document discusses the International Council for Harmonisation of Technical Requirements for Pharmaceuticals for Human Use (ICH) guidelines. It provides an overview of the regulatory bodies and research-based industries involved in different regions. It then describes the process of harmonization through various steps including consensus building, confirmation of agreement, regulatory consultation and discussion, acceptance as a harmonized guideline, and implementation. It lists several Q, S, and E series guidelines covering topics like quality, safety, and efficacy.

    Copyright:

    © All Rights Reserved
    Download as PPTX, PDF, TXT or read online from Scribd
    Download as pptx, pdf, or txt
    101 views31 pages

    Ich and Qsem

    Uploaded by

    Vaishnavi Karmveer
    The document discusses the International Council for Harmonisation of Technical Requirements for Pharmaceuticals for Human Use (ICH) guidelines. It provides an overview of the regulatory bodies and research-based industries involved in different regions. It then describes the process of harmonization through various steps including consensus building, confirmation of agreement, regulatory consultation and discussion, acceptance as a harmonized guideline, and implementation. It lists several Q, S, and E series guidelines covering topics like quality, safety, and efficacy.

    Copyright:

    © All Rights Reserved
    Download as PPTX, PDF, TXT or read online from Scribd
    Download as pptx, pdf, or txt
    of 31

    ICH Guidelines

    Regulatory bodies and research-based


    Industry
    Region Regulatory Body Research Based Industry

    • -

    Japan MHLW - Ministry of JPMA - Japan


    Health, Labour and Pharmaceutical
    Welfare Manufacturers
    Association
    Europe EU European Union EFPIA - European
    Federation of
    Pharmaceutical
    Industries and
    Associations
    USA FDA - Food and Drug PhRMA - Pharmaceutical
    Administration Research and
    Manufacturers of
    America
    PROCESS OF HARMONISATION
    • Formal ICH procedure
    • Question and answer procedure
    • Revision procedure
    • Maintenance procedure.
    PROCESS OF HARMONISATION
    Step 1: Consensus building(Agreement)

    • The process of unanimity starts when the Steering


    Committee acquires a Concept Paper as a new topic. Step
    1 is started when the EWG begin the preparation of a
    unanimity draft of the technical document, depending on
    the objectives set out in the Concept Paper.
    • Work is conducted via e-mail, telephonic conferences and
    web conferences. If supported by the Steering committee,
    the EWG will also meet face to face at the 2 years SC
    meetings. Meanwhile reports on the progress of the draft
    technical document are made to the SC on a regular
    interval
    Step 2a: Confirmation of six-party unanimity
    on the technical document
    • Step 2a is reached when the Steering Committee
    accepts based on the report of the EWG, that there
    is enough scientific consensuses on the technical
    issues for the Technical Document to proceed to the
    next stage of regulatory consultation.
    • The unanimity text approved by the Steering
    Committee is signed-off by the Steering Committee
    as the Step 2a Final Technical Document.
    Step 2b: Espousal of the draft Guideline:

    • Based on the technical document, the three


    ICH regulatory members will take the actions
    they deem essential to develop the “draft
    Guideline”. The unanimity text approved by
    the three regulatory ICH members is signed-
    off by the three regulatory ICH members as
    Step 2b Draft
    Step 3: Regulatory consultation and
    Discussion:
    • Stage I: Regional regulatory consultation
    • Stage II: Discussion of regional consultation
    comments:
    • Stage III: Finalisation of Step 3 Experts Draft
    Guideline
    Step 4: Acceptance of an ICH Harmonised
    Tripartite Guideline:
    • Step 4 is completed when the Steering Committee
    accepts, on the basis of the report from the
    Regulatory Chair and the regulatory Rapporteur
    of the EWG, that there is sufficient unanimity on
    the draft guideline. Step 4 is reached when the
    Step 4 Final Document is signed-off by the SC
    signatories for the regulatory members of ICH as
    an ICH Harmonised Tripartite Guideline at Step 4
    of the ICH procedure.
    Step 5: Implementation:
    • After completing Step 4, the harmonised
    tripartite Guideline moves immediately to
    the final step of the process that is the
    regulatory execution or Step 5. Step 5 is
    accomplished according to the same
    national/regional procedures that apply to
    other regional regulatory requirements, in
    the, USA, Japan and the European Union.
    Objective

    1. More efficient use of human, animal and


    material resources.
    2. Elimination of unnecessary and unreasonable
    delay in the global development and
    availability of new medicines while
    maintaining safeguards on quality, safety and
    efficacy.
    3. Regulatory obligations to protect public health .
    Q- Series Guidelines
    Q1A - Q1F Stability
    Q2(R1)- Validation of analytical procedure
    Q3A - Q3D Impurities
    Q4A - Q4B Pharmacopoeias
    Q5A - Q5E Quality of Biotechnological Products
    Q6A- Q6B Specifications
    Q7 Good Manufacturing Practice
    Q8 Pharmaceutical Development
    Q9 Quality Risk Management
    Q10 Pharmaceutical Quality System
    Q11 Development and Manufacture of Drug Substances
    Q12 Lifecycle Management
    Q1A - Q1F Stability

    Q1A(R2) Stability Testing of New Drug Substances and


    Products Q1A
    Q1B Stability Testing : Photostability Testing of New
    Drug Substances and Products
    Q1C Stability Testing for New Dosage Forms
    Q1D Bracketing and Matrixing Designs for Stability
    Testing of New Drug Substances and Products
    Q1E Evaluation of Stability Data
    Q1F Stability Data Package for Registration Applications
    in Climatic Zones III and IV
    Q2(R1)- Validation of analytical procedure

    Text & methodology for analytical method


    validation for stability study.
    Q3A - Q3D Impurities
    Q3A(R2) Impurities in New Drug Substances
    Q3B(R2) Impurities in New Drug Products
    Q3C(R6) Impurities: Guideline for Residual Solvents
    Q3C(R7) Impurities: Guideline for Residual Solvents
    Q3D Guideline for Elemental Impurities
    Q3D(R1) Revision of Q3D Cadmium Inhalation PDE
    Q3D(R2) Revision of Q3D for cutaneous and
    transdermal products
    Q3D training Implementation of Guideline for
    Elemental Impurities
    Q4A - Q4B Pharmacopoeias

    Q4A Pharmacopoeial Harmonization


    Q4B Evaluation and Recommendation of Pharmacopoeial Texts for
    Use in the ICH Regions
    Q4B Annex 1R1 Residue on Ignition/Sulphated Ash General
    Chapter
    Q4B Annex 2R1 Test for Extractable Volume of Parenteral
    Preparations General Chapter
    Q4B Annex 3R1 Test for Particulate Contamination: Sub-Visible
    Particles General Chapter
    Q4B Annex 4AR1 Microbiological Examination of Non-Sterile
    Products: Microbial Enumeration Tests General Chapter
    Q4B Annex 4BR1 Microbiological Examination of Non-Sterile
    Products: Tests for Specified Micro-Organisms General Chapter
    Q4B Annex 4CR1 Microbiological Examination of Non-Sterile Products:
    Acceptance Criteria for Pharmaceutical Preparations and Substances for
    Pharmaceutical Use General Chapter
    Q4B Annex 5R1 Disintegration Test General Chapter
    Q4B Annex 6 Uniformity of Dosage Units General Chapter
    Q4B Annex 7R2 Dissolution Test General Chapter
    Q4B Annex 8R1 Sterility Test General Chapter
    Q4B Annex 9R1 Tablet Friability General Chapter
    Q4B Annex 10R1 Polyacrylamide Gel Electrophoresis General Chapter
    Q4B Annex 11 Capillary Electrophoresis General Chapter
    Q4B Annex 12 Analytical Sieving General Chapter
    Q4B Annex 13 Bulk Density and Tapped Density of Powders General
    Chapter
    Q4B Annex 14 Bacterial Endotoxins Test General Chapter
    Q4B FAQs Frequently Asked Questions
    Q5A - Q5E Quality of Biotechnological Products
    Q5A(R1) Viral Safety Evaluation of Biotechnology
    Products Derived from Cell Lines of Human or Animal
    Origin Q5A
    Q5B Analysis of the Expression Construct in Cells Used for
    Production of r-DNA Derived Protein Products
    Q5C Stability Testing of Biotechnological/Biological
    Products
    Q5D Derivation and Characterization of Cell Substrates
    Used for Production of Biotechnological/Biological
    Products
    Q5E Comparability of Biotechnological/Biological
    Products Subject to Changes in their Manufacturing
    Process
    Q6A- Q6B Specifications

    Q6A Specifications : Test Procedures and


    Acceptance Criteria for New Drug Substances and
    New Drug Products: Chemical Substances

    Q6B Specifications : Test Procedures and


    Acceptance Criteria for
    Biotechnological/Biological Products
    Q7 Good Manufacturing Practice

    Q7 Good Manufacturing Practice Guide for Active


    Pharmaceutical Ingredients Q7A

    Q7 Q& As Questions and Answers: Good


    Manufacturing Practice Guide for Active
    Pharmaceutical Ingredients
    Q8 Pharmaceutical Development

    Q8(R2) Pharmaceutical Development

    Q8/9/10 Q&R4 Q8/Q9/Q10 - Implementation


    Q9 Quality Risk Management

    Q9 Quality Risk Management


    Q8/9/10 Q&AsR4 Q8/Q9/Q10 - Implementation
    Q10 Pharmaceutical Quality System

    Q10 Pharmaceutical Quality System

    Q8/9/10 Q&AsR4 Q8/Q9/Q10 – Implementation.


    Q11 Development and Manufacture of Drug
    Substances

    Q11 Development and Manufacture of Drug


    Substances (Chemical Entities and
    Biotechnological/Biological Entities)

    Q11 Q&As Questions & Answers: Selection and


    Justification of Starting Materials for the
    Manufacture of Drug Substances
    Q12 Lifecycle Management

    Q12 Technical and Regulatory Considerations for


    Pharmaceutical Product Lifecycle Management.
    Safety Guidelines:
    S1A - S1C Carcinogenicity Studies
    S2 Genotoxicity Studies
    S3A - S3B Toxicokinetics and Pharmacokinetics
    S4 Toxicity Testing
    S5 Reproductive Toxicology
    S6 Biotechnological Products
    S7A - S7B Pharmacology Studies
    S8 Immunotoxicology Studies
    S9 Nonclinical Evaluation for Anticancer Pharmaceuticals
    S10 Photosafety Evaluation
    S11 Nonclinical Pediatric Safety
    Efficacy Guidelines
    E1 Clinical Safety for Drugs used in Long-
    Term Treatment
    E2A - E2F Pharmacovigilence
    E3 Clinical Study Reports
    E4 Dose-Response Studies
    E5 Ethnic Factors
    E6 Good Clinical Practice
    E7 Clinical Trials in Geriatric Population
    E8 General Considerations for ClinicalzTrials
    E9 Statistical Principles for Clinical Trials
    E10 Choice of Control Group in Clinical Trials
    E11 - E11A Clinical Trials in Pediatric
    Population
    E12 Clinical Evaluation by Therapeutic
    Category
    E14 Clinical Evaluation of QT
    E15 Definitions in Pharmacogenetics /
    Pharmacogenomics
    E16 Qualification of Genomic Biomarkers
    E17 Multi-Regional Clinical Trials
    E18 Genomic Sampling
    E19 Safety Data Collection

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