Presentation is loading. Please wait.

Presentation is loading. Please wait.

ICH GUIDELINES Himanshu Kamboj Assistant professor.

Published byHimanshu Kamboj Modified over 4 years ago

Similar presentations

Presentation on theme: "ICH GUIDELINES Himanshu Kamboj Assistant professor."— Presentation transcript:

1 ICH GUIDELINES Himanshu Kamboj Assistant professor

2 CONTENTS ICH and ICH guidelines Need Origin of ICH Evolution of ICH ICH members Steps of ICH Categories of ICH guidelines

3 ICH AND ICH GUIDELINES ICH stands for “International Conference on Harmonization of Technical Requirements for Registration of Pharmaceuticals for Human Use”. Which is international non-profit Association,which is unique in bringing together the regulatory authorities and pharmaceutical industries. Where European Union, Japan and the USA involve in scientific and technical discussions of the testing procedures required to assess and ensure the safety, quality and efficacy of medicines These are the three pillars on which the health of the patients depend.

4 ICH Guidelines accepted as law in several Countries to ensure and access the Q,S,E of medicines but are only used as guidance for the U.S Food and Drug Administration. Each regulatory co-sponsor implements the guidelines according to its National or Regional requirements. They are intended to be used in combination with any regional requirements.

5 NEED Many time-consuming and expensive test procedures, in order to market new products, internationally. Over rising costs of health care making safe and efficacious new treatments available to patients in need. Divergence in technical requirements from country to country.

6 ORIGIN OF ICH Harmonization of regulatory requirements was pioneered by the EU, Europe, in the 1980s as the Europe move towards the development of single market. The success achieved in Europe demonstrated that harmonization was feasible. At the same time there were discussions between Europe, Japan and the US on possibilities for harmonization. The birth of ICH took place at a meeting in April 1990. Topics selected for harmonization would be divided into safety,quality and efficacy to reflect the three criteria which are the basis for approving and authorizing new medicinal products.

7 EVOLUTION OF ICH First decade : significant progress in the development of ICH Guidelines on Safety, Quality and Efficacy topics and also work on a number of important multidisciplinary topics. Second decade: implementation of ICH Guidelines in the ICH regions. Expand communication and information on ICH Guidelines with other regions Third decade : extending the benefits of harmonization beyond the ICH regions. Training,as well as active participation of other regions in Guideline development is seen as key in this effort.

8 ICH MEMBERS EU EFPIA (European federation of pharmaceutical industries’ associations). MHLW (Ministry of health, Labor and welfare, Japan). JPMA (Japan Pharmaceuticals manufacturers Association). US FDA. PhRMA(pharmaceutical research and manufacturers association). Observers : WHO, TPP(Canada). International federation of Pharmaceutical manufacturer’s association.

9 STEPS OF ICH STEP 1: Building Scientific Consensus STEP 2: Agreeing on Draft Text STEP 3: Consulting Regional Regulatory Agencies STEP 4: Adopting Harmonized Guidelines STEP 5: Implementing Guidelines in ICH Regions

10 CATEGORIES OF ICH GUIDELINES The guidelines of ICH are broadly categorized into four types. 1) Quality guidelines. 2) Safety guidelines. 3) Efficacy guidelines. 4) Multidisciplinary guidelines.

11 QUALITY : Harmonization achievements in the Quality area include such as the conduct of stability studies, defining relevant thresholds for impurities testing and a more flexible approach to pharmaceutical quality based on Good Manufacturing Practice (GMP) risk management. Q1A - Q1F :Stability Q2 : Analytical Validation Q3A - Q3D : Impurities Q4 - Q4B : Pharmacopoeias Q5A - Q5E : Quality of Biotechnological Products Q6A- Q6B : Specifications Q7 : Good Manufacturing Practice Q8 : Pharmaceutical Development Q9 : Quality Risk Management Q10 : Pharmaceutical Quality System Q11 : Development and Manufacture of Drug Substances Q12 : Lifecycle Management Q13 : Continuous Manufacturing of Drug Substances and Drug Products Q14 : Analytical Procedure Development

12 SAFETY : ICH has produced a comprehensive set of safety Guidelines to potential risks like carcinogenicity, genotoxicity and reprotoxicity etc., S1A - S1C : Carcinogenicity Studies S2 : Genotoxicity Studies S3A - S3B : Toxicokinetics and Pharmacokinetics S4 : Toxicity Testing S5 : Reproductive Toxicology S6 : Biotechnological Products S7A - S7B : Pharmacology Studies S8 : Immunotoxicology Studies S9 : Nonclinical Evaluation for Anticancer Pharmaceuticals S10 : Photosafety Evaluation S11 : Nonclinical Pediatric Safety

13 EFFICACY : The work carried out by ICH under the Efficacy heading is concerned with the design, conduct, safety and reporting of clinical trials. It also covers novel types of medicines derived from biotechnological processes and the use of pharmacogenetics / genomics techniques to produce better targeted medicines. E1 : Clinical Safety for Drugs used in Long-Term Treatment E2A - E2F : Pharmacovigilance E3 : Clinical Study Reports E4 : Dose-Response Studies E5 : Ethnic Factors E6 : Good Clinical Practice E7 :Clinical Trials in Geriatric Population E8 : General Considerations for Clinical Trials E9 :Statistical Principles for Clinical Trials E10 : Choice of Control Group in Clinical Trials E11 - E11A : Clinical Trials in Pediatric Population E12 :Clinical Evaluation by Therapeutic Category E14 :Clinical Evaluation of QT E15 :Definitions in Pharmacogenetics / Pharmacogenomics E17 : Multi-Regional Clinical Trials E18 : Genomic Sampling

14 MULTIDISCPLINARY : These are the cross-cutting topics which do not fit uniquely into one of the Quality, Safety and Efficacy categories. It includes the ICH medical terminology (MedDRA), the Common Technical Document (CTD) and the development of Electronic Standards for the Transfer of Regulatory Information (ESTRI). M1 : MedDRA Terminology M2 : Electronic Standards M3 : Nonclinical Safety Studies M4 : Common Technical Document. M5 : Data Elements and Standards for Drug Dictionaries M6 : Gene Therapy M7 : Mutagenic impurities M8 : Electronic Common Technical Document (eCTD) M9 : Biopharmaceutics Classification System-based Biowaivers M10 : Bioanalytical Method Validation

15 THANKU YOU

Download ppt "ICH GUIDELINES Himanshu Kamboj Assistant professor."

Similar presentations

6th European Patients’ Rights Day The EMA Geriatric Medicines Strategy and the empowered aging patient Francesca Cerreta EMA (European Medicines Agency)

6th European Patients’ Rights Day The EMA Geriatric Medicines Strategy and the empowered aging patient Francesca Cerreta EMA (European Medicines Agency)
17 September 2007ISO TC215 WG6 Brisbane1 Identification of Medicinal Products & Pharmacovigilance Task Forces.

17 September 2007ISO TC215 WG6 Brisbane1 Identification of Medicinal Products & Pharmacovigilance Task Forces.
EPAA Conference 5 November 2007 Georgette LALIS Enterprise and Industry DG European Commission The international dimension of regulatory acceptance.

EPAA Conference 5 November 2007 Georgette LALIS Enterprise and Industry DG European Commission The international dimension of regulatory acceptance.
EPAA Annual conference November 2007 1 Regulatory acceptance of alternative approaches for pharmaceuticals Jean-Marc Vidal Safety & Efficacy of Human Medicines.

EPAA Annual conference November Regulatory acceptance of alternative approaches for pharmaceuticals Jean-Marc Vidal Safety & Efficacy of Human Medicines.
Regulatory Clinical Trials Clinical Trials. Clinical Trials Definition: research studies to find ways to improve health Definition: research studies to.

Regulatory Clinical Trials Clinical Trials. Clinical Trials Definition: research studies to find ways to improve health Definition: research studies to.
Www.gf-associates.co.uk Regulatory Framework Leigh Shaw, Director.

Regulatory Framework Leigh Shaw, Director.
Common Terminology Criteria for Adverse Events (CTCAE) v.4: Updating a Cancer Research Standard Ann Setser 1, Ranjana Srivastava 2, Lawrence Wright 1,

Common Terminology Criteria for Adverse Events (CTCAE) v.4: Updating a Cancer Research Standard Ann Setser 1, Ranjana Srivastava 2, Lawrence Wright 1,
ICH E-5 Overview and Current Topics Mamoru Narukawa.

ICH E-5 Overview and Current Topics Mamoru Narukawa.
U.S. DEPARTMENT OF HEALTH AND HUMAN SERVICES NATIONAL INSTITUTES OF HEALTH Working with FDA: Biological Products and Clinical Development Critical Path.

U.S. DEPARTMENT OF HEALTH AND HUMAN SERVICES NATIONAL INSTITUTES OF HEALTH Working with FDA: Biological Products and Clinical Development Critical Path.
The ICH E5 Question and Answer Document Status and Content Robert T. O’Neill, Ph.D. Director, Office of Biostatistics, CDER, FDA Presented at the 4th Kitasato-Harvard.

The ICH E5 Question and Answer Document Status and Content Robert T. O’Neill, Ph.D. Director, Office of Biostatistics, CDER, FDA Presented at the 4th Kitasato-Harvard.
A Case Study in the Value of Harmonisation Yoshikazu HAYASHI Deputy Director Evaluation and Licensing Division Pharmaceutical & Food Safety Bureau Ministry.

A Case Study in the Value of Harmonisation Yoshikazu HAYASHI Deputy Director Evaluation and Licensing Division Pharmaceutical & Food Safety Bureau Ministry.
2014-01-22Stefan Franzén Introduction to clinical trials.

Stefan Franzén Introduction to clinical trials.
Knowledge Update Clinical documentation: from preclinical studies to drug registration Split, 12 September 2008.

Knowledge Update Clinical documentation: from preclinical studies to drug registration Split, 12 September 2008.
Clinical Trials of Traditional Herbal Medicines In India Y.K.Gupta Professor & Head, Department of Pharmacology, All India Institute of Medical Sciences,

Clinical Trials of Traditional Herbal Medicines In India Y.K.Gupta Professor & Head, Department of Pharmacology, All India Institute of Medical Sciences,
Training Workshop on Pharmaceutical Development with a Focus on Paediatric Medicines / 15-19 October 2007 1 |1 | Regulatory Requirement on Dossier of Medicinal.

Training Workshop on Pharmaceutical Development with a Focus on Paediatric Medicines / October |1 | Regulatory Requirement on Dossier of Medicinal.
CDER IND/NDA Reviews Guidance, The Common Technical Document and Good Review Practice John K. Leighton, Ph.D., DABT CDER/FDA.

CDER IND/NDA Reviews Guidance, The Common Technical Document and Good Review Practice John K. Leighton, Ph.D., DABT CDER/FDA.
Structure of Dossier of Medicinal Product- Q part

Structure of Dossier of Medicinal Product- Q part
Biopharmaceutical Regulatory Requirements 40. Marketing Authorization for New Chemical Entities Health Canada’s (HC) Therapeutic Products Directorate.

Biopharmaceutical Regulatory Requirements 40. Marketing Authorization for New Chemical Entities Health Canada’s (HC) Therapeutic Products Directorate.
Eureka Pre-Clinical Investigation Animal toxicology Animal pharmacokinetics/ pharmacodynamics Clinical Investigation Phase I Safety and pharmacology Phase.

Eureka Pre-Clinical Investigation Animal toxicology Animal pharmacokinetics/ pharmacodynamics Clinical Investigation Phase I Safety and pharmacology Phase.
Justina A. Molzon, MS Pharm, JD

Justina A. Molzon, MS Pharm, JD

Similar presentations

Ads by Google