Preparing the CMC Section for NDAs/INDs/CTDs

This course will provide participants with a thorough understanding of the requirements for each CMC/Quality section of the Common Technical Document (CTD), the format to be used for NDAs, including preparation of the Quality Overall Summary (Module 2). It will also present techniques for making the CMC submission easy to review, including sample tables and figures, and discuss how to address issues during meetings with FDA and NDA review.

ICH Process and CTD Organization

• Minimum and optimum granularity
• Impact of Established Conditions on preparation of new NDA
• Differences between Draft ICH Q12 Pharmaceutical Product Lifecycle Management and existing FDA guidances

Requirements for the Drug Substance (Module 3 of CTD)

S.1 General Information:

• Nomenclature, structure, general properties

S.2 Manufacture

• Use of contractors vs in-house manufacturers
• Detail necessary in manufacturing process description
• Determination of critical steps and controls
• Reprocessing vs rework
• Use of alternative processes
• Justification for starting materials
• When to validate manufacturing process
• Manufacturing process development (Q11)
• Development of Control Strategy

S.3 Characterization

• Potential for polymorphs
• Specified/unspecified impurities vs identified/unidentified impurities
• Impurity thresholds
• Genotoxic impurities

S.4 Control of the Drug Substance

• Universal vs specific tests in specifications
• Requirements for alternative analytical procedures
• Transfer of analytical procedures
• When to validate analytical procedures
• Importance of batch analyses table
• How to justify specifications

S.5 Reference Standards

• Use of primary vs secondary reference standards

S.6 Container Closure System

• Suitability of container closure system

S.7 Stability

• Requirements for primary registration stability studies
• Rationale for forced degradation/stress testing
• Extension of retest dating period
• Requirements for post-approval stability studies

Drug Master Files (DMFs)

• What is a DMF
• Types of DMFs
• Why are DMFs used
• How are DMFs used
• Role play DMF process
• What goes into DMF vs NDA

Requirements for the Drug Product (Module 3 of CTD)

P.1 Description and Composition

• Naming of salts

P.2 Pharmaceutical Development

• Drug substance information needed for pharmaceutical development
• Impact of excipient choice and concentration
• Rationale for overage vs overfill
• Elements of container closure suitability
• Container closure development vs container closure information in P.6
• Rationale for preservative systems

P.3 Manufacture

• Use of contractors vs in-house manufacturers
• Detail necessary in manufacturing process description
• When to validate manufacturing processes

P.4 Control of Excipients

• Information required for excipients
• Justification for excipient specifications
• Requirements for novel excipients

P.5 Control of the Drug Product

• Universal vs specific tests in specifications
• Drug product vs drug substance impurities in specifications
• Justification for specifications

P.6 Reference Standards

• Need for impurity reference standards

P.7 Container Closure Systems

• Requirements for primary vs secondary vs functional secondary container closures

P.8 Stability

• Requirements for primary registration stability studies
• When to bracket or matrix stability studies
• Need for forced degradation/stress testing
• Need for in-use studies
• Need for cycling studies
• Extension of expiration dating period
• Requirements for post-approval stability studies

CMC Appendices/Regional Information

• Executed batch records to be provided
• FDA analytical method validation
• Comparability protocol content and benefit

Quality Overall Summary (Module 2 of CTD)

• When and how to prepare Module 2

FDA Interactions

• How to prepare for FDA meetings
• CMC-specific meeting or general meeting
• How to respond to FDA questions

"Instructor went through the content very well and kept things moving. She adapted well to participants questions."

Susan T., Sr. Medical Writer, MMS Holdings

"One of the best courses I've taken, I learned a great deal."

Jiang L., Principal Investigator, Enanta Pharmaceuticals

"This was the first course I have taken with CfPIE and it was very interactive and informative. It was a great experience and starting point for me."

Harpreet K., Senior Chem Mgr, Dalton Pharma Services

"The course was very well designed and covered the material nicely."

Jesper V., Scientist, Zealand Pharma

"The course director is a very good communicator and exceptional instructor. She was very patient in explaining the various modules and coordinating the discussions. I learned much more with this course and can say that my knowledge regarding the CMC preparation has improved significantly after attending this course. I will be on the lookout for other courses offered by CfPIE"

Sheetal M., Principal Scientist, Purdue Pharma L.P.

"The course director was an excellent presenter. I am a project manager and took this course as a way to get an overview of the CMC. I learned so much! This will be very useful as reference as I lead my project teams in Drug Development. She did an excellent job managing and answering questions from SMES from all areas - Analytical Regulatory, Formulation, DP Development, DS Development, Quality."

Karen B., Sr. Project Manager, Pfizer

"An excellent seminar for everyone coordinating, writing or reviewing the CMC sections of drug substance and drug product NDAs/INDs for small molecules."

A. Agidotan, Manager, PharmaLex GmbH

"This was an excellent instructor with great real-world experiences who presented the information very clearly!"

David D., Scientist, Upsher Smith Laboratories

"This course was a great class for me! Previously, I had only been involved with the early R&D activities and never have written any submission sections. This course helped me clarify the relationships between ICH guidelines and NDA submissions, as well as delineate between the different types of ICH guidelines."

David A., Global Program Manager, Synthes

"I thought this course was excellent and very relevant to my work. It will benefit me greatly as I move closer to preparing for NDA filing. The instructor encouraged questions and discussions which provided different perspectives and other companies' experiences/practices. This was very beneficial as well."

Elizabeth G., Research Scientist, BMS

"The course director was very knowledgeable in presenting her material. She was able to provide real life examples to support her discussion. The course notes will be a valuable reference tool for future use."

Sylvie A., Project Leader, Regulatory Affairs, Sanofi-Aventis Canada

"I am involved in Research and Process Development of API. By attending this excellent course I really could see what my role was in the overall regulatory filings process and how important it was from the quality perspective."

Hitesh B., Manager, R&D, United Therapeutic