Module 3

Module 3 Christa Clasen Ankara, 6./7. April 2006

Module 3 • 3.1 Table of Content • 3.2 Body of Data • 3.2.S Drug Substance • 3.2.P Drug Product • 3.2.A Appendices • 3.2.R Regional Information • 3.3 Literature References Christa Clasen Ankara, 6./7. April 2006

3.2.S Drug Substance • 3.2.S.1 General Information • 3.2.S.2 Manufacture • 3.2.S.3 Characterisation • 3.2.S.4 Control of drug substance • 3.2.S.5 Reference Standards or Materials • 3.2.S.6 Container Closure System • 3.2.S.7 Stability Christa Clasen Ankara, 6./7. April 2006

3.2.S.1 General Information • 3.2.S.1.1 Nomenclature INN, Compendial name, chemical name, other name, laboratory codes, CAS – number • 3.2.S.1.2 Structure Physical form, structural formula (incl. stereochemistry) • 3.2.S.1.3 General Properties Physico-chemical characterisation (solubility, physical characteristics, polymorphism, other) Christa Clasen Ankara, 6./7. April 2006

3.2.S.2 Manufacture • 3.2.S.2.1 Manufacturer • 3.2.S.2.2 Description of Manufacturing Process and Process Controls • 3.2.S.2.3 Controls of Materials • 3.2.S.2.4 Control of Critical Steps and Intermediates • 3.2.S.2.5 Process Validation and/or Evaluation • 3.2.S.2.6 Manufacturing Process Development Christa Clasen Ankara, 6./7. April 2006

3.2.S.2 Manufacture • 3.2.S.2.1 Manufacturer • Address office • Address plant Company profile is not obligatory • If starting materials/ or used intermediates already contains a key-structure of the final drug substance, information of those manufacturer(s) are required Christa Clasen Ankara, 6./7. April 2006

3.2.S.2 Manufacture • 3.2.S.2.2 Description of Manufacturing Process and Process Controls Applicant‘s Part: • Synthetic route: overview • Flow chart • Brief narrative description of the process Christa Clasen Ankara, 6./7. April 2006

3.2.S.2 Manufacture 3.2.S.2.2 Description of Manufacturing Process and Process Controls Restricted Part: • Synthetic route: Overview • Flow chart including molecular formula, weights, yields, chemical structures of starting materials, intermediates, reagents and drug substance reflecting stereochemistry, operating conditions and used solvents • Narrative description of the process covering in more detail the information given in the flow-chart Christa Clasen Ankara, 6./7. April 2006

3.2.S.2 Manufacture • 3.2.S.2.3 Control of Materials • List of used raw materials identifying where each material is used in the process. • Control of starting materials (Specifications, Description of Test methods) • Control of solvents and other reagents (Specifications, Description of Test methods) • If starting materials already contains the key-structure of the final API, a synthesis-outline (including solvents, reagents, catalysts, potential Impurities) for these starting materials are required Christa Clasen Ankara, 6./7. April 2006

3.2.S.2. Manufacture • 3.2.S.2.4 Control of Critical Steps and Intermediates • Control of Intermediates (Specifications, Description of test methods) • Tests and acceptance criteria (with justification including experimental data) performed at critical steps identified in 3.2.S.2.2 Christa Clasen Ankara, 6./7. April 2006

3.2.S.2 Manufacture • 3.2.S.2.5 Process Validation and/or Evaluation Process Validation studies should be included (only for aseptic processes or sterilisation) In any case: Validation studies have to be perfomed and needs to be available at request Christa Clasen Ankara, 6./7. April 2006

3.2.S.2 Manufacture • 3.2.S.2.6 Manufacturing Process Development A description and discussion about the significant changes/improvements to the manufacturing process and/or manufacturing site of the drug substance is awaited Christa Clasen Ankara, 6./7. April 2006

3.2.S.3 Characterisation • 3.2.S.3.1. Eludication of Structure and other Characteristics • Evidence of the chemical structure (elemental analysis, mass spectrum, 1H-NMR, 13C-NMR, IR, UV, other) • Potential isomerism • Stereochemistry • Polymorphism Christa Clasen Ankara, 6./7. April 2006

3.2.S.3 Characterisation • 3.2.S.3.2. Impurities • List of potential impurities originating from the route of synthesis • List of potential impurities arising during the production and purification • List of actual existing impurities (synthesis by-products, degradation products) • List of potential residual solvents • List of actual residual solvents in API • Evidence of the chemical structure (elemental analysis, mass spectrum, 1H-NMR, 13C-NMR, IR, UV, other) for each Impurity Christa Clasen Ankara, 6./7. April 2006

3.2.S.4 Control of Drug Substance • 3.2.S.4.1 Specification • According to which pharmacopoeia, in-house • Characteristics • Identification tests • Purity tests (including limits for known, total, unidentified single and unidentified total) • Other tests • Assay Christa Clasen Ankara, 6./7. April 2006

3.2.S.4 Control of Drug Substance • 3.2.S.4.2 Analytical Procedures Reference to pharmacopoeia, or detailed description of all tests • 3.2.S.4.3 Validation of Analytical Procedures Validation of all used methods according to ICH Guidelines Q2A and Q2B (if they are not pharmacopoeial) Christa Clasen Ankara, 6./7. April 2006

3.2.S.4 Control of Drug Substance • 3.2.S.4.4 Batch analysis • Batches tested (date of manufacture, place of manufacture, batch size) • Results of tests (3 - 5 consecutive certificates of analysis) • 3.2.S.4.5 Justification of the drug substance specification • Comments on the Choice of Routine Tests • Justification of Specification Limits Christa Clasen Ankara, 6./7. April 2006

3.2.S.5. Reference Standards or Materials • List of used Reference Standards or Materials • Preparation of Reference Standards, if appropriate • Elucidation of Structure for synthesized Materials • Specification for Reference materials • Description of Test Methods • Validation of Analytical Methods if not covered by 3.2.S.4.3 Christa Clasen Ankara, 6./7. April 2006

3.2.S.6 Container Closure System • Description of Container Closure System including Identity of Materials and their specification • Discussion of suitability of Packaging material Christa Clasen Ankara, 6./7. April 2006

3.2.S.7 Stability • 3.2.S.7.1. Stability Summaries and Conclusions • Program of stability studies (including forced degradation studies if appropriate, e.g. testing parameters, packaging material, storage conditions, batch number, manufacturing date, batch size • Conclusion Christa Clasen Ankara, 6./7. April 2006

3.2.S.7 Stability • 3.2.S.7.2 Post-approval Stability Protocol and Stability Commitment Program of stability study including testing parameters, packaging material, storage conditions, batch number, manufacturing date, batch size, which will be performed post-approval Christa Clasen Ankara, 6./7. April 2006

3.2.S.7 Stability • 3.2.S.7.3 Stability data Results of: • Long-term study (initial, 3, 6, 9, 12, 18, 24, 36 months) for at least 3 batches • Accelerated study (initial, 1, 2, 3, 6 months) for the same batches as long-term study • Intermediate study (initial, 3, 6, 9, 12, 18, 24, 36 months) for at least 3 batches, if appropriate • Forced degradation study (alkaline conditions, acidic conditions, higher temperature, oxidative condition, light) Christa Clasen Ankara, 6./7. April 2006

3.2.P Drug Product • 3.2.P.1 Description and Compostion of the Drug Product • 3.2.P.2 Pharmaceutical Development • 3.2.P.3 Manufacture • 3.2.P.4 Control of Excipients • 3.2.P.5 Control of Drug Product • 3.2.P.6 Reference Standards or Materials • 3.2.P.7 Container Closure System • 3.2.P.8 Stability Christa Clasen Ankara, 6./7. April 2006

3.2.P.1 Description and Composition of the Drug Product • Description of dosage form • List of components and their amount • Function of components • Reconstitution diluent(s) Christa Clasen Ankara, 6./7. April 2006

3.2.P.2 Pharmaceutical Development • 3.2.P.2.1 Components of Drug Product • 3.2.P.2.2 Drug Product • 3.2.P.2.3 Manufacturing Process Development • 3.2.P.2.4 Container Closure System • 3.2.P.2.5 Microbiological Attributes • 3.2.P.2.6 Compatibility Christa Clasen Ankara, 6./7. April 2006

3.2.P.2 Pharmaceutical Development • 3.2.P.2.1 Components of the Drug Product • 3.2.P.2.1.1 Drug Substance • Compatibility with Excipients • Key physicochemical Characteristics • 3.2.P.2.1.2 Excipients • Justification of Choice Christa Clasen Ankara, 6./7. April 2006

3.2.P.2 Pharmaceutical Development • 3.2.P.2.2 Drug Product • 3.2.P.2.2.1 Formulation Development Brief summary, which is describing the development • 3.2.P.2.2.2 Overages Justification of Overages • 3.2.P.2.2.3 Physicochemical and Biological Properties Christa Clasen Ankara, 6./7. April 2006

3.2.P.2 Pharmaceutical Development • 3.2.P.2.3 Manufacturing Process Development Selection and optimisation of the manufacturing process with its particular critical steps • 3.2.P.2.4 Container Closure System Suitability of the Container Closure System used for storage, transportation and drug product Christa Clasen Ankara, 6./7. April 2006

3.2.P.2 Pharmaceutical Development • 3.2.P.2.5 Microbiological AttributesMicrobiological Attributes should be discussed • 3.2.P.2.6 Compatibility Compatibility of with reconstitution diluent(s) Christa Clasen Ankara, 6./7. April 2006

3.2.P.3 Manufacture • 3.2.P.3.1 Manufacturer(s) • 3.2.P.3.2 Batch Formula • 3.2.P.3.3 Description of Manufacturing Process and Process Controls • 3.2.P.3.4 Controls of Critical Steps • 3.2.P.3.5 Process Validation and/or Evaluation Christa Clasen Ankara, 6./7. April 2006

3.2.P.3 Manufacture • 3.2.P.3.1 Manufacturer(s) Name, address and responsibility of each manufacturer • 3.2.P.3.2 Batch Formula Batch formula incl. all components with amounts and references Christa Clasen Ankara, 6./7. April 2006

3.2.P.3 Manufacture • 3.2.P.3.3 Description of Manufacturing Process and Process Controls • Flow diagram • Narrative description of the manufacturing process • Process parameters • Proposals for justification of reprocessing of materials Christa Clasen Ankara, 6./7. April 2006

3.2.P.3 Manufacture • 3.2.P.3.4 Controls of Critical Steps and Intermediates • Critical Steps: Test and acceptance criteria • Intermediates: Information of quality and control • 3.2.P.3.5 Process validation and/or evaluation Description, documentation, results of validation and/or evaluation studies Christa Clasen Ankara, 6./7. April 2006

3.2.P.4 Control of Excipients • 3.2.P.4.1 Specifications • 3.2.P.4.2 Analytical Procedures • 3.2.P.4.3 Validation of Analytical Procedures • 3.2.P.4.4 Justification of Specification • 3.2.P.4.5 Excipients of Human or Animal Origin • 3.2.P.4.6 Novel Excipients Christa Clasen Ankara, 6./7. April 2006

3.2.P.4 Control of Excipients • 3.2.P.4.1 Specification Specification should be provided • 3.2.P.4.2 Analytical Procedure Analytical Procedures should be provided • 3.2.P.4.3 Validation of Analytical Procedures Information about Validation Christa Clasen Ankara, 6./7. April 2006

3.2.P.4 Control of Excipients • 3.2.P.4.4 Justification of Specification Justification for the proposed specification for the excipients • 3.2.P.4.5 Excipients of Human or Animal Origin Information regarding adventitious agens should be provided. • 3.2.P.4.6 Novel Excipients For excipients used the first time or by a new route of administration detailed information according to the Drug Substance format should be provided. Christa Clasen Ankara, 6./7. April 2006

3.2.P.5 Control of Drug Product • 3.2.P.5.1 Specification(s) • 3.2.P.5.2 Analytical Procedures • 3.2.P.5.3 Validation of Analytical Procedures • 3.2.P.5.4 Batch Analysis • 3.2.P.5.5 Characterisation of Impurities • 3.2.P.5.6 Justification of Specification(s) Christa Clasen Ankara, 6./7. April 2006

3.2.P.5 Control of Drug Product • 3.2.P.5.1 Specification(s) Specification(s) should be provided • 3.2.P.5.2 Analytical Procedures Analytical Procedures should be provided Christa Clasen Ankara, 6./7. April 2006

3.2.P.5 Control of Drug Product • 3.2.P.5.3 Validation of Analytical Procedures Analytical Validation should be provided • 3.2.P.5.4 Batch Analysis Descripition of batches and results of batch analysis should be provided Christa Clasen Ankara, 6./7. April 2006

3.2.P.5 Control of Drug Product • 3.2.P.5.5 Characterisation of Impurities Characterisation of Impurities  if not provided in 3.2.S.3.2 (Impurities) • 3.2.P.5.6 Justification of Specification(s) Justification of proposed specification(s) should be provided Christa Clasen Ankara, 6./7. April 2006

3.2.P.6 Reference Standards or Materials Information about reference standards or materials should be provided  if not provided in 3.2.S.5 „Reference standards or materials“ Christa Clasen Ankara, 6./7. April 2006

3.2.P.7 Container Closure System • Identity and specification of each primary packaging components • Brief description of non-functional secondary packaging component • Information about functional secondary packaging component Christa Clasen Ankara, 6./7. April 2006

3.2.P.8 Stability • 3.2.P.8.1 Stability Summary and Conclusion • 3.2.P.8.2 Post-approval Stability Protocol and Stability Commitment • 3.2.P.8.3 Stability Data Christa Clasen Ankara, 6./7. April 2006

3.2.P.8 Stability • 3.2.P.8.1 Stability Summary and Conclusion The Stability Summary should include: • Types of Studies • Results of Studies • Conclusion with respect to storage conditions and shelf-life Christa Clasen Ankara, 6./7. April 2006

3.2.P.8 Stability • 3.2.P.8.2 Post-approval Stability Protocol Post-approval stability protocoll and the stability commitment should be provided • 3.2.P.8.3 Stability Data • Presentation of the results in an appropriate format • Information of analytical procedures incl. validation Christa Clasen Ankara, 6./7. April 2006

3.2.A Appendices • 3.2.A.1 Facilities and Equipment • 3.2.A.2 Adventitious Agents Safety Evaluation • 3.2.A.3 Novel Excipients Christa Clasen Ankara, 6./7. April 2006

3.2.R Regional Information (EU) • Process Validation Scheme for Drug Product • Medical Devices • Certificate(s) of Suitability • TSE templates (place in 3.2.A.2) Christa Clasen Ankara, 6./7. April 2006

Module 3

Module 3

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Module 3

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