T-Cell Dependent Immunogenicity of Protein Therapeutics Pre-clinical Assessment and Mitigation–Updated Consensus and Review 2020

Vibha Jawa; Frances Terry; Jochem Gokemeijer; Shibani Mitra-Kaushik; Brian J. Roberts; Sophie Tourdot; Anne S. De Groot; Anne S. De Groot

doi:10.3389/fimmu.2020.01301

Frontiers in Immunology (Jun 2020)

T-Cell Dependent Immunogenicity of Protein Therapeutics Pre-clinical Assessment and Mitigation–Updated Consensus and Review 2020

Vibha Jawa,
Frances Terry,
Jochem Gokemeijer,
Shibani Mitra-Kaushik,
Brian J. Roberts,
Sophie Tourdot,
Anne S. De Groot,
Anne S. De Groot

Affiliations

Vibha Jawa: Predictive and Clinical Immunogenicity, PPDM, Merck & Co., Kenilworth, NJ, United States
Frances Terry: EpiVax, Inc., Providence, RI, United States
Jochem Gokemeijer: Discovery Biotherapeutics, Bristol-Myers Squibb, Cambridge, MA, United States
Shibani Mitra-Kaushik: Biologics Development, Sanofi, Framingham, MA, United States
Brian J. Roberts: EpiVax, Inc., Providence, RI, United States
Sophie Tourdot: BioMedicine Design, Pfizer Inc., Andover, MA, United States
Anne S. De Groot: EpiVax, Inc., Providence, RI, United States
Anne S. De Groot: Center for Vaccines and Immunology, University of Georgia, Athens, GA, United States

DOI: https://doi.org/10.3389/fimmu.2020.01301
Journal volume & issue: Vol. 11

Abstract

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Immune responses to protein and peptide drugs can alter or reduce their efficacy and may be associated with adverse effects. While anti-drug antibodies (ADA) are a standard clinical measure of protein therapeutic immunogenicity, T cell epitopes in the primary sequences of these drugs are the key drivers or modulators of ADA response, depending on the type of T cell response that is stimulated (e.g., T helper or Regulatory T cells, respectively). In a previous publication on T cell-dependent immunogenicity of biotherapeutics, we addressed mitigation efforts such as identifying and reducing the presence of T cell epitopes or T cell response to protein therapeutics prior to further development of the protein therapeutic for clinical use. Over the past 5 years, greater insight into the role of regulatory T cell epitopes and the conservation of T cell epitopes with self (beyond germline) has improved the preclinical assessment of immunogenic potential. In addition, impurities contained in therapeutic drug formulations such as host cell proteins have also attracted attention and become the focus of novel risk assessment methods. Target effects have come into focus, given the emergence of protein and peptide drugs that target immune receptors in immuno-oncology applications. Lastly, new modalities are entering the clinic, leading to the need to revise certain aspects of the preclinical immunogenicity assessment pathway. In addition to drugs that have multiple antibody-derived domains or non-antibody scaffolds, therapeutic drugs may now be introduced via viral vectors, cell-based constructs, or nucleic acid based therapeutics that may, in addition to delivering drug, also prime the immune system, driving immune response to the delivery vehicle as well as the encoded therapeutic, adding to the complexity of assessing immunogenicity risk. While it is challenging to keep pace with emerging methods for the preclinical assessment of protein therapeutics and new biologic therapeutic modalities, this collective compendium provides a guide to current best practices and new concepts in the field.

Published in Frontiers in Immunology

ISSN: 1664-3224 (Online)
Publisher: Frontiers Media S.A.
Country of publisher: Switzerland
LCC subjects: Medicine: Internal medicine: Specialties of internal medicine: Immunologic diseases. Allergy
Website: http://journal.frontiersin.org/journal/immunology

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