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    Chemistry, Manufacturing and Controls Requirements: Exhibit 1: CMC Requirements For A New Pharmaceutical

    Uploaded by

    Pranav Patel
    CMC requirements

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    © All Rights Reserved
    Download as PDF, TXT or read online from Scribd

    Chemistry, Manufacturing and Controls Requirements: Exhibit 1: CMC Requirements For A New Pharmaceutical

    Uploaded by

    Pranav Patel
    226 views3 pages
    CMC requirements

    Original Title

    CMC Requirements

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    CMC requirements

    Copyright:

    © All Rights Reserved
    Download as PDF, TXT or read online from Scribd
    Download as pdf or txt
    226 views3 pages

    Chemistry, Manufacturing and Controls Requirements: Exhibit 1: CMC Requirements For A New Pharmaceutical

    Uploaded by

    Pranav Patel
    CMC requirements

    Copyright:

    © All Rights Reserved
    Download as PDF, TXT or read online from Scribd
    Download as pdf or txt
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    The document outlines the chemistry, manufacturing and controls (CMC) requirements for new pharmaceuticals according to International Conference on Harmonisation (ICH) guidelines, including drug substance and product information as well as stability testing requirements.

    The CMC portion should include information about the drug substance, manufacturing process, characterization, specifications, container closure system, and stability data.

    The purpose of stability testing is to determine how the drug substance or product performs under different environmental conditions and to establish a re-test period or shelf-life as well as recommended storage conditions.

    Chemistry,

    manufacturing and
    controls requirements

    The chemistry, manufacturing and controls (CMC) section is a very important part of any clinical trial or marketing
    application. Drugs can be denied marketing approval if the quality of the product and the manufacturing process
    cannot be shown to be of a sufficiently high standard to satisfy regulators.
    The following outlines the key parts of the CMC portion of a file, as per the International Conference on
    Harmonisation (ICH) requirements.

    Exhibit 1: CMC requirements for a new pharmaceutical

    Drug substance

    Section

    Inclusions

    General information

    Recommended international non-proprietary name (INN),


    compendial name (if relevant), chemical name, company
    or lab code, other non-proprietary names, chemical
    abstracts service (CAS) registry number, structure, general
    physicochemical and other relevant properties.

    Manufacture

    Name, address and responsibility of each manufacturer


    involved in process, description of manufacturing process
    and controls, control of materials, controls of critical steps
    and intermediates, process validation and/or evaluation,
    manufacturing process development.

    Characterisation

    Elucidation of structure and other characteristics,


    impurities.

    Control of drug substance

    Specification, analytical procedures, validation of analytical


    procedures, batch analyses, justification of specification.

    Reference standards or materials

    Drug product

    Container closure system

    Description, identity and specifications.

    Stability

    Stability summary and conclusions, post-approval stability


    protocol and stability commitment, stability data.

    Description and composition

    Description, composition, type of container closure system.

    Pharmaceutical development

    Components of the drug product (drug substance,


    excipients), formulation development, overage,
    physicochemical and biological properties, manufacturing
    process development, container closure system,
    microbiological attributes, compatability.

    Manufacture

    Manufacturers name, batch formula, description of


    manufacturing process and process controls, controls of
    critical steps and intermediates, process validation and/or
    evaluation.

    MaRS Copyright 2010

    Control of excipients

    Specifications, analytical procedures, validation of


    analytical procedures, justification of specifications,
    excipients of animal or human origin, novel excipients.

    Control of drug product

    Specifications, analytical procedures, validation of


    analytical procedures, batch analyses, characterization of
    impurities, justification of specifications.

    Reference standards or materials


    Container closure system
    Stability

    Stability summary and conclusion, post-approval stability


    protocol and stability commitment, stability data.

    Source: International Conference on Harmonisation, Common Technical Document for the Registration of
    Pharmaceuticals for Human Use [Guideline M4Q(R1)], http://www.ich.org/LOB/media/MEDIA556.pdf

    The ICH guideline Q1A(R2) (Stability Testing of New Drug Substances and Products) defines the stability data
    package required for new drug substances and products submitted for approval in each of the major regions that
    accept the ICH guidelines (i.e., US, Japan and EU).

    Stability testing
    The purpose of stability testing is to determine how the drug substance or product performs under different
    environmental conditions such as temperature, humidity and light. It also establishes a re-test period for the drug
    substance or a shelf-life for the drug product, as well as recommended storage conditions.

    Drug substance stability testing


    At least three batches of a drug substance should be tested. The ICH guideline Q1A(R2) states that, Batches must
    be manufactured at least to pilot scale by the same synthetic route as production batches and using a method of
    manufacture and procedure that simulates the final process to be used for production batches. The stability testing
    should be conducted on products that have been stored in the same type of container that is intended for market
    use (e.g., bottles, blister packages).
    For drug substances with a proposed twelve-month re-test period, ideally batches should be tested every three
    months over the first year and every six months over the second year, and annually thereafter.
    Under accelerated storage conditions, in a six-month study, batches should be tested at the zero-, three- and sixmonth mark.

    Drug product stability testing


    Stability testing should be conducted from three primary batches of the same formulation and packaged in the
    same container closure system as intended for market use. The manufacturing process should simulate the one
    used for production batches and should provide a product of the same quality and that meets the same release
    specifications as the batches intended for the market. Two of the three batches should be pilot scale batches; the
    third one can be smaller, if justified. Where possible, the three batches should be made using different batches of
    drug substances.
    Note that additional stability and compatibility studies may be required if a product is to be combined with either
    another product or diluted in a vehicle for administration.
    Exhibits 2, 3 and 4 below detail the general stability data required for drug substances and drug products, as well as
    the stability requirements when they are refrigerated or frozen.

    MaRS Copyright 2010

    Exhibit 2: General stability data required for drug substance or drug product
    Study

    Storage condition

    Minimum time period covered by


    data at time of submission

    Long-term**

    25C+2C/60% RH +5% RH
    or
    30C+2C/65% RH +5% RH

    12 months

    Intermediate*

    30C+2C/65% RH +5% RH

    6 months

    Accelerated

    40C+2C/75% RH +5% RH

    6 months

    ** It is up to the applicant to decide whether long-term stability studies are performed at which of the two conditions.
    * If 30C+2C/65% RH+5% RH is the long-term condition, there is no intermediate condition.

    Source: International Conference on Harmonisation, Stability Testing of New Drug Substances and Products
    [Guideline Q1A(R2)], http://www.ich.org/LOB/media/MEDIA419.pdf

    Exhibit 3: Stability requirements for refrigerated drug substance or drug product


    Study

    Storage condition

    Minimum time period covered by


    data at time of submission

    Long-term

    5C+3C

    12 months

    Intermediate

    25C+2C/60% RH +5% RH

    6 months

    Source: International Conference on Harmonisation, Stability Testing of New Drug Substances and Products
    [Guideline Q1A(R2)], http://www.ich.org/LOB/media/MEDIA419.pdf

    Exhibit 4: Stability requirements for frozen drug substance or drug product


    Study

    Storage condition

    Minimum time period covered by


    data at time of submission

    Long-term

    -20C+5C

    12 months

    Source: International Conference on Harmonisation, Stability Testing of New Drug Substances and Products
    [Guideline Q1A(R2)], http://www.ich.org/LOB/media/MEDIA419.pdf

    MaRS Copyright 2010

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