Sol Ruiz, PhD, Spain

Similar documents
Optimizing the Development of Biosimilars Using PK/PD: Recent Scientific and Regulatory Advances

Closed Workshop on biosimilar monoclonal antibodies and immunogenicity of monoclonal antibodies October 2011 Dr Christian K Schneider, MD

Vladimir Hanes, MD, USA

Biosimilar Monoclonal- a reality

Panama City, Panama April, 12-15, Marcelo Mario Matos Moreira. The Brazilian Health Surveillance Agency (ANVISA)

Professor Andrea Laslop, MD, Austria

Biosimilar mabs Clinical issues Regulatory perspective

<RENFLEXIS> <Ministry of Food and Drug Safety>

Baek, Kyung-min. Recombinant Protein Products Division. Ministry of Food and Drug Safety

ACG Public Forum. Join ACG, the FDA, and EMA for a discussion on biosimilars and IBD. Monday, 12:45 pm 2:15 pm

What next? Manufacture the biosimilar product

Biosimilars Scientific Challenges and Implications

ACG Public Forum. Join ACG, the FDA, and EMA for a discussion on biosimilars and IBD. Monday, 12:45 pm 2:15 pm

Biological and Functional Analysis of

DRAFT GUIDELINE ON SIMILAR MEDICINAL PRODUCTS CONTAINING RECOMBINANT INTERFERON ALPHA

Guideline on similar medicinal products containing somatropin. Draft agreed by BMWP March Adopted by CHMP for release for consultation May 2005

Overcoming Challenges in the Emerging Biosimilar Landscape

IPRF Biosimilars Working Group Reflection Paper on Extrapolation of Indications in Authorization of Biosimilar Products

IPRF Biosimilars Working Group Reflection Paper on Extrapolation of Indications in Authorization of Biosimilar Products

Biosimilars Scientific and Regulatory Considerations

Guideline on similar biological medicinal products containing recombinant granulocyte-colony stimulating

Guideline on similar biological medicinal products containing interferon beta

Implications for Preclinical and Clinical Programs. Novartis Pharmaceuticals Oncology Business Unit June 2, 2011

Revised Immunogenicity Guideline: Assays and methods- Presentation of the draft guideline and introduction of the topics for discussion

London Medicines Evaluation Network Review

Thijs J Giezen, PharmD, MSc, PhD The Netherlands

Biosimilars in the EU

Biosimilars China Guideline. Dr Dr Michel Mikhail

fact sheet 3 Introduction to Biosimilars & Regulatory Requirements

Develop A Highly Similar" Biosimilar Compound: Lessons Learnt

COMMITTEE FOR HUMAN MEDICINAL PRODUCTS (CHMP)

COMMITTEE FOR MEDICINAL PRODUCTS FOR HUMAN USE (CHMP)

COMMITTEE FOR MEDICINAL PRODUCTS FOR HUMAN USE (CHMP)

Sandoz Biopharmaceuticals. Sandoz Biosimilars. From concept to reality

Andrew Nesbitt, PhD. Disclaimer 10/10/2014. Determining the Immunogenicity of Biologics: a Tricky Problem. Employee of UCB ן

Trial-design in biosimilar research: Equivalence or non-inferiority design

Professor Francisco José de Abajo, MD, MPH, PhD, Spain

Current Trends and Future of Biosimilars

Harmonizing clinical trials for Biogenerics. Dr. Akhilesh Sharma M.D.;C Clin. Research & P.V. (UCBC - USA & Luton - UK)

COMMITTEE FOR MEDICINAL PRODUCTS FOR HUMAN USE (CHMP)

An update on development strategies of recently approved biosimilars in Europe. Johanna Mielke

FDA Public Hearing: Approval Pathway for Biosimilar. Products. November 2-3, 2010

Biosimilar regulation in Republic of Korea and Asia-Pacific Economic Cooperation (APEC) developments

Risk-based testing for anti-drug neutralizing antibodies during development of biological therapeutics

Submission of comments on Guideline on Similar Biological Medicinal Products (CHMP/437/04 Rev1)

COMMITTEE FOR MEDICINAL PRODUCTS FOR HUMAN USE (CHMP)

MEDICINES CONTROL COUNCIL

Guideline for the quality, safety and efficacy of follow-on biological medicinal products

Biosimilar Monoclonal Antibodies: Registration Requirements. Henry M. J. Leng

An MHRA perspective on bioassays

Regulatory Issues and Drug Product Approval for Biopharmaceuticals

Biosimilar Development Clinical Investigator Considerations

Jan Willem van der Laan

A Physician s consideration towards Biosimilars. João Eurico Fonseca

Expectations for Bioassays - An Assessor s View

How much evidence is provided prior to approval? An updated systematic review of biosimilar applications in Europe

Sharmila et al. International Journal of Drug Regulatory Affairs; 2017, 5(1), ISSN: Available online at

Matthias Grossmann, MD PhD Principal Consultant Early Phase 2013 PAREXEL International

Guideline on Similar Biological Medicinal Products

Expectations for Analytical Characterisation in the Evaluation of Biosimilarity: A Regulator`s Perspective

KFDA Regulatory Framework on Biopharmaceuticals - Focus on Biosimilar

Biologicals and biosimilars in the wind - what is new?

CHALLENGES AND SOLUTIONS TO RECEPTOR OCCUPANCY STUDIES BY FLOW CYTOMETRY

Medicines Agency EMA & Biosimilar update: Trends from marketing authorisation applications, scientific advice procedures and policies

Guideline for the Quality, Safety, and Efficacy Assurance of Follow-on Biologics

Update on the new immunogenicity guideline in the EU

THE BIOSIMILARS LANDSCAPE: STRATEGIES FOR CLINICAL AND COMMERCIAL SUCCESS

Antibody-Mediated Effector Function: Learning and Challenges from Early Discovery to Development

Immunogenicity: Impact on the Design of Clinical Trials for Biosimilars

1. Introduction Purpose and scope Terminology Special considerations for characterization and quality assessment 101

Niklas Ekman, PhD, Finland

Interested parties (organisations or individuals) that commented on the draft document as released for consultation.

Biosimilars today or tomorrow?

This presentation was developed by the Government & Industry Affairs Committee of the Crohn s & Colitis Foundation of America

Promise and Pitfalls of MicrobiomeModulating Methods for Inflammatory

Similar biological medicinal product

5 key characteristics

Considerations in Product Development with Advanced Therapies and Cancer Vaccines

Why even have this talk? Disclosures. What will biosimilars mean for us? Annual Revenue Due to Adalimumab. Biosimilars 2017: What We Need to Know

NDA Advisory Services Ltd

Clinical Trials for Biotechnology Medicines

Cancer Vanguard. An introduction to Biosimilars

Requirements for demonstrating biosimilarity of monoclonal antibodies

Professor Ahmed H Al-jedai, PharmD, MBA, BCPS, FCCP, FAST, Saudi Arabia

Nonclinical Data to Support FIH Clinical Trials for Cancer Immunotherapies. Whitney S. Helms, PhD IOM, February 29,2016

PLANNING FOR SUCCESS: A CMC STRATEGY FOR BIOSIMILARS

Pharmacist Rana Musa Al-ali (Malkawi) MSc (Pharmaceutical Quality Assurance) Registration Department/JFDA

The Future Role of Biosimilars: An Unknown Frontier in IBD Treatment

Johanna Andrea García Cortes, MSc, Colombia

Preclinical Development of Biologics: Case-by-case, so get off of my case!

The revised EU (CHMP) immunogenicity guidance on therapeutic proteins. Meenu Wadhwa, Biotherapeutics Group, NIBSC

CADTH CANADIAN DRUG EXPERT COMMITTEE FINAL RECOMMENDATION

ACG Public Forum. Join ACG, the FDA, and EMA for a discussion on biosimilars and IBD. Monday, 12:45 pm 2:15 pm

OBP s MARJORIE SHAPIRO ON ANALYTICAL SIMILARITY IN BIOSIMILAR APPROVAL

Pharmacology. Chatchai Chinpaisal, Ph.D. Department of Pharmacology and Toxicology, Faculty of Pharmacy, Silpakorn University.

Quality issues in biosimilars Some thoughts

Future Directions in IBD: Treatments & Approaches

The Future has Arrived: Biosimilars

Identification of Critical Product Quality Attributes: Impact of Product Variants on Safety and Efficacy

8. Clinical Trial Assessment Phase II

Transcription:

GaBI Scientific Meetings ROUNDTABLE ON BIOSIMILARS Pharmacovigilance, Traceability, Immunogenicity 15 November 2016, Real Academia Nacional de Farmacia, Madrid, Spain Sol Ruiz, PhD, Spain Head of Sector, Biotechnology and Advanced Therapies, Spanish Agency for Medicines and Medical Devices (Agencia Española de Medicamentos y Productos Sanitarios) Chair, Biosimilar Medicinal Product Working Party, European Medicines Agency Member of the Committee for Advanced Therapies, European Medicines Agency Co-opted member of the Committee for Medicinal Products for Human Use, Quality and Safety (biological)

GaBI Scientific Meetings ROUNDTABLE ON BIOSIMILARS Pharmacovigilance, Traceability, Immunogenicity 15 November 2016, Real Academia Nacional de Farmacia, Madrid, Spain EMA approval requirements on biosimilars: clinical aspects Sol Ruiz, PhD, Spain 15 November 2016

1. extensive characterization (physicochemical, biological) 2. in vitro functional activity (analyzing all possible MoA of the molecule) 3.efficacy and safety (most sensitive population to detect differences)

1. extensive characterization (physicochemical, biological) 2. in vitro functional activity (analyzing all possible MoA of the molecule) 3.efficacy and safety (most sensitive population to detect differences)

Primary objective: to show comparable PK in a sufficiently sensitive and homogeneous population. Healthy volunteers OK (patients, if a toxic MoA)

Use of multiple PD markers recommended (if possible) Explore dose-concentration-response or time-response relationships PD markers as pivotal evidence for comparable efficacy if: Clear dose-response relationship shown At least one PD marker is an accepted surrogate marker and can be related to patient outcome If not Step 2

Adequately powered, randomised, parallel group comparative clinical trial, preferably double-blind, normally equivalence trials. Deviation from relevant efficacy guidelines should be justified Most sensitive patient population and clinical EP preferred Comparative S data (immunogenicity) Extrapolation of indications: possible; based on the overall evidence of comparability

A large -250 patients-, multiple-dose, PK study in patients with ankylosing spondylitis showed BE of the biosimilar and the reference product (supportive evidence for comparable safety, efficacy, and immunogenicity) Equivalent efficacy and comparable safety and immunogenicity (randomized, controlled clinical trial in rheumatoid arthritis; 606 patients)

FLIXABI (infliximab)

2015

2015

Extrapolation of data is already an established scientific and regulatory principle that has been exercised for many years, for example, in the case of major changes in the manufacturing process of originator biologicals.

44

Factors to considered for extrapolation: Clinical experience with the reference product MoA/active site(s) of the active substance in each indication (including its degree of certainty) Target receptors involved Differences in the safety/immunogenicity profile between the therapeutic indications, including considerations on patient-related factors (comorbidities, comedication, immunologic status) and disease-related factors (reactions related to the target cells, e.g lysis of tumor cells). The degree to which the functional moieties of the molecule can be analytically characterized and compared.

EXTRAPOLATION OF INDICATIONS Points to consider Overall evidence of comparability Remaining uncertainties from the data provided Acceptable safety profile (including immunogenicity)

1. extensive characterization (physicochemical, biological) 2. in vitro functional activity (analyzing all possible MoA of the molecule) 3.efficacy and safety (most sensitive population to detect differences)

Additional in vitro studies: Critical to show comparability

Extensive analytical tests showed physicochemical and structural comparability except for a small difference in the proportion of afucosylated forms (associated with increased binding affinity to the FcγRIIIa receptor). Comparable binding of the test and reference product to the soluble and/or the membranebound TNFα (main MoA), functions mediated by transmembrane binding, including reverse signaling and apoptosis.

Similar inhibition of the direct effects of TNFα on epithelial cells that play an important role in Crohn s disease Similar induction of regulatory macrophages is implicated as a mode of action of infliximab in IBD

1. extensive characterization (physicochemical, biological) 2. in vitro functional activity (analyzing all possible MoA of the molecule) 3.efficacy and safety (most sensitive population to detect differences)

TRYPTIC MAP CD spectra

MS CZE

Oligosaccharide map

FUNCTIONAL ANALYSIS antiviral activity antiproliferative activities (using different cell lines) immunomodulatory activities receptor binding formation of activated IFN stimulated gene factor complex IFN-beta inducible mrnas

sruiz@aemps.es

2024 © businessdocbox.com Privacy Policy | Terms of Service | Feedback