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Pharmaceutical Nomenclature Issues and challenges

Pharmaceutical Nomenclature Issues and challenges. Moheb M. Nasr, Ph.D. Acting Director Office of New Drug Chemistry (ONDC) OPS, CDER, FDA Advisory Committee for Pharmaceutical Sciences (ACPS) October 22, 2003. Pharmaceutical Nomenclature Issues and challenges. FDA Perspective

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Pharmaceutical Nomenclature Issues and challenges

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  1. Pharmaceutical NomenclatureIssues and challenges Moheb M. Nasr, Ph.D. Acting Director Office of New Drug Chemistry (ONDC) OPS, CDER, FDA Advisory Committee for Pharmaceutical Sciences (ACPS) October 22, 2003

  2. Pharmaceutical Nomenclature Issues and challenges FDA Perspective Orally Disintegrating Tablets (ODT) Topical Dosage Form Classification - an Update Committee Discussions Dan Boring, R.Ph.,Ph.D. Frank Holcombe, Jr., Ph.D. Lucinda Buhse, Ph.D. ACPS, October 22, 2003

  3. Issues and challenges • Impact on regulatory decisions, marketing, drug development, and the public • Nomenclature development (scientific and regulatory challenges) • How to do it right the first time? • Is a new dosage form needed or is it just a minor modification in an existing dosage form that can be handled by labeling? • How to establish definitions and criteria for new dosage forms? • Do we need to have that many dosage forms? ACPS, October 22, 2003

  4. Issues and challenges • Coordination with different organizations and stakeholders • Definitions (descriptive and quantifiable attributes) • Refinement and/or replacement of older dosage forms • Pharmaceutical equivalence issues ACPS, October 22, 2003

  5. Questions for ACPS 1. What are the factors that the Agency should consider in determining (a) whether a new dosage form name is warranted and (b) how such a dosage form should be defined? 2. Is it reasonable or useful to include a quantifiable attribute when defining a dosage form or distinguishing between closely related dosage forms where appropriate? Can such an approach be viewed as too arbitrary in some cases and too rigid in other cases? ACPS, October 22, 2003

  6. Questions for ACPS 3. Is the proposed criterion, i.e., an in vitro disintegration time of less than 60 seconds, reasonable for defining an orally disintegrating tablet? 4. Has the update on topical dosage forms presented today addressed the questions/comments raised by the ACPS at the March 2003 meeting? ACPS, October 22, 2003

  7. FDA Perspective on Dosage Form Nomenclature Dr. Dan Boring, R.Ph., Ph.D. Review Chemist; Labeling Expert ONDC, OPS

  8. Nomenclature ofPharmaceutical Dosage Forms • Issues and challenges • Scientific • Regulatory • Marketing • Legal • Healthcare provider • Patient ACPS, October 22, 2003

  9. What is an Established Name? • The FD&C Act states “drug” only • Drug substance and/or drug product? • At CDER, an established name for both drug substance and drug product • In general, an established name for a drug product is: [(drug substance) (release characteristic) (route of administration) (dosage form)] • Today’s focus is on dosage form ACPS, October 22, 2003

  10. Definition ofa Pharmaceutical Drug Product • Drug Product is defined as a finished dosage form such as tablet, capsule or solution • What is a dosage form? • A dosage form could be defined as the physical form of a drug product at the point that it is introduced into the body, or, where final preparation is required before introduction into the body, the physical form of the drug product in the package that bears instructions for final preparation (private communication) • Dosage forms are non-proprietary ACPS, October 22, 2003

  11. Stakeholders • Innovators • Research, development, marketing, legal • FDA • OND, ONDC, ODS, COS, NSC • USP • Expert Comm on Nomenclature and Labeling • Healthcare providers and patients • Not direct participants ACPS, October 22, 2003

  12. FDA Nomenclature Issues • New drugs • No USP monograph exists • Is a new name necessary? • Is it nomenclature or labeling? • Generic drugs • Compliance with USP monograph? • Is a compendial name being developed? • Will name allow proper product selection for substitution? • Name definition should not allow generic manufacturers to substitute a new dosage form for a RLD • OTC drugs • Product selection by patient ACPS, October 22, 2003

  13. Nomenclature Assessment Factors • Name must clearly identify the product • Name promotes accurate recognition without risk of medication errors • Name meets database, indexing and listing needs • Name consistent with precedents (i.e., systems) • Name should not provide an advantage through exclusive proprietary technology ACPS, October 22, 2003

  14. Challenges • Will a new name serve long-term needs? • Is an older term still accurate? • Is a developing new term appropriate? • Can objective standards be developed to define a new dosage form? • How should name development be coordinated (innovator, FDA, USP)? • Global harmonization? • Implementation? ACPS, October 22, 2003

  15. New Dosage Forms and Drug Delivery Systems • Orally disintegrating tablets • Tablets for suspension • Liposomes • Microspheres • Films? • Iontophoretic systems? ACPS, October 22, 2003

  16. DefiningOrally Disintegrating Tablets Frank Holcombe, Jr. Ph.D. Associate Director for Chemistry Office of Generic Drugs, OPS

  17. Current Definitions of ODT • FDA definition “A solid dosage form containing medicinal substances which disintegrates rapidly, usually within a matter of seconds, when placed upon the tongue” • USP Stimuli proposal “A solid oral dosage form that disintegrates rapidly in the mouth” ACPS, October 22, 2003

  18. Desired Characteristics and Benefits of ODT • Oral disintegration • Rapid disintegration • No chewing or liquids necessary • Provides improved route of administration and increased compliance for certain patient populations ACPS, October 22, 2003

  19. Issues Concerning ODT • Limited experience – similarity of all initial products • Expansion in product variations due to changes in • Technologies • Formulations • Additional drug products • Target market population ACPS, October 22, 2003

  20. Issues Concerning ODT • Format of suitable definition • Should address both the desired characteristics and control of extent of product range • Must address: • Method of administration • Objective criteria (limits for disintegration time) ACPS, October 22, 2003

  21. Issues Concerning ODT • Disintegration evaluation • In-vivo testing (subjective, objective) • In-vitro testing (objective) • Variety of methods • Results may be method dependent ACPS, October 22, 2003

  22. In-vitro Testing Methods • Applicant in-house methods (proprietary) • FDA laboratory method (static) • USP Chapter <701> Disintegration (dynamic) ACPS, October 22, 2003

  23. In-vitro Testing Results • Static: 1-78 sec • Dynamic: 1-69 sec • Most products in 1 to 30 sec range • No data correlating in-vivo and in-vitro disintegration times ACPS, October 22, 2003

  24. In-vitro Testing Results ACPS, October 22, 2003

  25. FDA Proposal • A revision of the ODT definition to include in-vitro disintegration method and acceptance criteria (USP <701>, < 60 sec) Objective: To provide criteria (based on original expectations) for distinguishing orally disintegrating tablets from other tablet forms ACPS, October 22, 2003

  26. Topical Dosage Form Classification – an Update Lucinda Buhse, Ph.D. Acting Director Division of Pharmaceutical Analysis Office of Testing and Research, OPS

  27. ACPS, October 22, 2003

  28. Advisory Committee Input • No need to include appearance and feel (e.g., greasy, non-greasy) • Definitions should be based on the vehicle • Ointments and suspensions could be classified as lotions (an overused term) • Do not make cream a default definition and do not separate creams using hydrophilic-vs-hydrophobic • Use detailed rheological evaluation (e.g., yield values) to distinguish gels and/or lotions from creams • Reconsider criteria used to classify gels ACPS, October 22, 2003

  29. CDER Activities • Evaluation of ACPS input • Consultations with Dr. Arthur Kibbe • Analysis of liquid/semi-solid borderline products based on more extensive rheological evaluation • Examination of optical properties and compositions of gels ACPS, October 22, 2003

  30. Rheological Evaluation Sample Yield Value (D/cm2) 1 50 29 90 62 125 61 160 36 195 50 200 51 525 4 600 32 660 Conformstocontainer Does not conform to container ACPS, October 22, 2003

  31. ACPS, October 22, 2003

  32. Questions for ACPS 1. What are the factors that the Agency should consider in determining (a) whether a new dosage form name is warranted and (b) how such a dosage form should be defined? 2. Is it reasonable or useful to include a quantifiable attribute when defining a dosage form or distinguishing between closely related dosage forms where appropriate? Can such an approach be viewed as too arbitrary in some cases and too rigid in other cases? ACPS, October 22, 2003

  33. Questions for ACPS 3. Is the proposed criterion, i.e., an in vitro disintegration time of less than 60 seconds, reasonable for defining an orally disintegrating tablet? 4. Has the update on topical dosage forms presented today addressed the questions/comments raised by the ACPS at the March 2003 meeting? ACPS, October 22, 2003

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