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    Unnati Garg CMC & CTD (Final

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    Unnati Garg
    This document provides an overview of chemistry, manufacturing, and controls (CMC) information and the common technical document (CTD) format required for regulatory submissions. CMC details how drugs are manufactured and ensures quality and consistency. The CTD standardizes application formats across regions into five modules covering administrative information, quality, nonclinical data, and clinical data. Module 3 specifically addresses quality including drug substance and product characteristics, manufacturing, and controls. The CTD format streamlines review processes and eliminates redundant submission requirements across authorities.

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    Unnati Garg CMC & CTD (Final

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    Unnati Garg
    48 views7 pages
    This document provides an overview of chemistry, manufacturing, and controls (CMC) information and the common technical document (CTD) format required for regulatory submissions. CMC details how drugs are manufactured and ensures quality and consistency. The CTD standardizes application formats across regions into five modules covering administrative information, quality, nonclinical data, and clinical data. Module 3 specifically addresses quality including drug substance and product characteristics, manufacturing, and controls. The CTD format streamlines review processes and eliminates redundant submission requirements across authorities.

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    Unnati Garg CMC & CTD (Final Doc)

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    This document provides an overview of chemistry, manufacturing, and controls (CMC) information and the common technical document (CTD) format required for regulatory submissions. CMC details how drugs are manufactured and ensures quality and consistency. The CTD standardizes application formats across regions into five modules covering administrative information, quality, nonclinical data, and clinical data. Module 3 specifically addresses quality including drug substance and product characteristics, manufacturing, and controls. The CTD format streamlines review processes and eliminates redundant submission requirements across authorities.

    Copyright:

    © All Rights Reserved
    Download as DOCX, PDF, TXT or read online from Scribd
    Download as docx, pdf, or txt
    48 views7 pages

    Unnati Garg CMC & CTD (Final

    Uploaded by

    Unnati Garg
    This document provides an overview of chemistry, manufacturing, and controls (CMC) information and the common technical document (CTD) format required for regulatory submissions. CMC details how drugs are manufactured and ensures quality and consistency. The CTD standardizes application formats across regions into five modules covering administrative information, quality, nonclinical data, and clinical data. Module 3 specifically addresses quality including drug substance and product characteristics, manufacturing, and controls. The CTD format streamlines review processes and eliminates redundant submission requirements across authorities.

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    © All Rights Reserved
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    of 7

    REGULATORY AFFAIRS

    CMC and CTD


    Unnati Garg
    M. Pharm (Pharmaceutics)
    A10647021011
    CHEMISTRY, MANUFACTURING AND CONTROL (CMC)

    INTRODUCTION
    The chemistry, manufacturing, and controls (CMC) section of a regulatory filing
    [investigational new drug (IND), IND amendments, IND annual reports, new drug
    application (NDA) or biologics license application (BLA), post approval CMC supplements,
    NDA annual reports] contains detailed information pertaining to the characteristics,
    manufacturing, and quality aspects of the drug substance and drug product.
    Why is there CMC?
     To assure that the drug sold to the public will have quality attributes similar to those
    of the drug demonstrated to be safe and effective.
     To assure that the quality of the drug meets appropriate standards and is consistent.
     To assure that the drug you are using is the drug described on the label.
    CMC Critical Elements
     How and where is the drug made?
     How are raw materials tested and monitored?
     What control procedures are in place to assure product consistency and quality?
     Are quality attributes adequately identified and characterized for the product?
     Are the test methods used to monitor product quality appropriate?
     How long does the product maintain its quality after it is made (shelf life/expiry)?
     CMC is one of the links that connects clinical batches to commercial batches.

    CMC is specific to the product


     Sterile injectable product – sterility and endotoxin concentration
     Controlled release product – release profile of active ingredient over time
     Oral tablet – dissolution profile
     Soluble powder for drinking water – moisture content as powder, solubility in water

    Process understanding is vital to Quality and Consistency


     Testing alone of the finished drug product is insufficient for control of product quality
     The manufacturer should know which steps and variables in the manufacturing
    process need to be controlled and why
     Process understanding is the foundation of a controlled manufacturing process
     A manufacturing Process under control exhibits consistency of product quality

    Over time, change is inevitable, but the product quality should either be constant or improve.
    Manufacturing changes impact drug quality, therefore CMC reviews the stability data from
    on- going studies.
    COMMON TECHNICAL DOCUMENT (CTD)
    The agreement to assemble all the Quality, Safety and Efficacy information in a common
    format (called CTD - Common Technical Document) has revolutionised the regulatory
    review processes, led to harmonised electronic submission that, in turn, enabled
    implementation of good review practices. For industries, it has eliminated the need to
    reformat the information for submission to the different ICH regulatory authorities.
    The CTD is organised into five modules. Module 1 is region specific and Modules 2, 3, 4 and
    5 are intended to be common for all regions. In July 2003, the CTD became the mandatory
    format for new drug applications in the EU and Japan, and the strongly recommended format
    of choice for NDAs submitted to FDA, United States.
    The Common Technical Document is divided into five modules:

    1. Administrative and prescribing information


    2. Overview and summary of modules 3 to 5
    3. Quality (pharmaceutical documentation)
    4. Preclinical (Pharmacology/Toxicology)
    5. Clinical – efficacy and safety (Clinical Trials)
    Detailed subheadings for each Module are specified for all jurisdictions. The contents of
    Module 1 and certain subheadings of other Modules will differ, based on national
    requirements.
    Module 2: CTD overviews and summaries
    Module 2 contains seven sections that should be maintained in the following order:
    2.1 Table of contents
    2.2 Introduction
    2.3 Quality Overall Summary
    2.4 Non-clinical Overview
    2.5 Clinical Overview
    2.6 Non-clinical Written and Tabulated Summaries
    2.7 Clinical Summary.
    Module 2.2: Introduction
    The introduction in Module 2.2 should be a general introduction to the IMP, including its
    pharmacological class, mode of action, and proposed clinical use. In general, the introduction
    should not exceed one page.
    Module 2.3: Quality overall summary
    The quality overall summary (QOS) is a summary of the chemical and pharmaceutical data in
    the dossier (including data for biological/biotechnological products). Guidance on the
    structure of the QOS is provided in ICH M4Q guidelines, with answers to the most common
    issues raised provided as a separate document. The structure of the QOS broadly follows the
    structure of the data included in Module 3. The QOS should not include information that has
    not already been included in Module 3 or in other parts of the CTD.
    Module 2.4: Non-clinical Overview and Module 2.6: Non-clinical Written and
    Tabulated Summaries
    The structure and content of Modules 2.4 and 2.6 are specified in the ICH M4S guidelines,
    with answers to the most common issues raised provided as a separate document. The main
    purpose of the Non-Clinical Written and Tabulated Summaries in Module 2.6 is to provide a
    comprehensive factual summary of the non-clinical information on pharmacology,
    pharmacokinetics, and toxicology. The Non-Clinical Written Summaries are generally in the
    region of 100–150 pages long. A total of 34 templates are provided for the preparation of the
    Tabulated Summaries in the ICH M4S guidelines
    Module 2.5: Clinical Overview and Module 2.7: Clinical Summary
    These modules are usually the documents a medical writer is most likely to be asked to write.
    The structure and content of Modules 2.5 and 2.7 are specified in the ICH M4E guidelines,
    with answers to common issues raised provided as a separate document. The Clinical
    Overview is a short document that provides a Critical Assessment of the clinical data,
    whereas the Clinical Summary is a longer document that focuses on data summarisation and
    integration.
    Module 3: Quality
    Module 3 presents the chemistry, manufacturing, and controls reports for the product
    included in the registration dossier. Full details of what should be included in Module 3 are
    provided in the ICH M4Q guideline. Sections on both drug substance and drug product are
    included in this module. The main headings in this section (that must not be altered) are as
    follows:
    3.1 Table of contents of Module 3
    3.2 Body of data
    3.2.S Drug Substance
    3.2.P+ Drug Product
    3.3 Literature references used in Module 3
    Module 4: Non-clinical study reports
    Module 4 presents the non-clinical reports included in the dossier. The structure and content
    of Module 4 is specified in the ICH M4S guidelines. The main headings in this section (that
    must not be altered) are as follows:
    4.1 Table of contents of Module 4
    4.2 Study reports
    4.2.1 Pharmacology
    4.2.2 Pharmacokinetics
    4.2.3 Toxicology
    4.3 Literature references used in Module 4.
    Module 5: Clinical study reports
    Module 5 presents the clinical reports included in the dossier. The structure and content of
    Module 5 is specified in the ICH M4E guidelines, which provided a specific placement of
    clinical study reports and related information to simplify preparation and review and to
    ensure completeness. The placement of a report is determined by the primary objective of the
    study, with each report appearing in only one section. If there are multiple objectives, the
    study should be cross-referenced in the various sections. The main headings in this section
    (that must not be altered) are as follows:
    5.1 Table of contents of Module 5
    5.2 Tabular listing of all clinical studies
    5.3 Clinical study reports
    5.3.1 Reports of biopharmaceutic studies
    5.3.2 Reports of studies pertinent to pharmacokinetics using human biomaterials
    5.3.3 Reports of human pharmacokinetic (PK) studies
    5.3.4 Reports of human pharmacodynamic (PD) studies
    5.3.5 Reports of efficacy and safety studies
    5.3.6 Reports of post-marketing experience
    5.3.7 Case report forms and individual patient listings
    5.4 Literature references.

    REFERENCES
    1. CMCsandGMPs.pptx (live.com)
    2. ICH Official web site : ICH
    3. Common Technical Document - Wikipedia
    4. Jordan D. An overview of the Common Technical Document (CTD) regulatory
    dossier. Medical Writing. 2014 Jun 1;23(2):101-5.

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