Reducing the Immunogenicity of Protein Therapeutics

Overview

Journal Curr Drug Targets

Publisher Bentham Science Publishers

Specialty Pharmacology

Date 2009 Feb 10

PMID 19199909

Citations 19

Authors

Masanori Onda

Affiliations

Soon will be listed here.

Abstract

Protein therapeutics, such as antibodies, enzymes and toxins, are very promising reagents for the treatment of human disease. However, many therapeutic proteins are known to elicit immune responses when administered to humans. Certain antibodies work by neutralization; others reduce drug efficacy. It is clear that helper T cells are an important factor in the development of class-switched and affinity-maturated anti-therapeutic protein antibodies. Elimination of the T cell epitope seems reasonable, but it is probably impossible to remove all T cell epitopes from protein drugs because T cell epitopes are closely related to the major histocompatibility complex (MHC) molecules, which are known to be highly polymorphic. Accordingly, a possible practical approach for reducing immunogenicity involves the removal of B cell epitopes. In this case, reducing the affinity between the antigen and the B cell receptor may reduce B cell activation, even though the T cell will still be activated. Also a B cell epitope is not restricted by MHC class II molecules. This review seeks to address the identification and the characterization of B cell epitopes, and reports on the development of strategies for reducing immune response with modified B cell epitopes.

Citing Articles

Computer-Assisted Design of Peptide-Based Radiotracers.

Patamia V, Zagni C, Brullo I, Saccullo E, Coco A, Floresta G Int J Mol Sci. 2023; 24(7).

PMID: 37047831 PMC: 10095039. DOI: 10.3390/ijms24076856.

Comprehensive deletion landscape of CRISPR-Cas9 identifies minimal RNA-guided DNA-binding modules.

Shams A, Higgins S, Fellmann C, Laughlin T, Oakes B, Lew R Nat Commun. 2021; 12(1):5664.

PMID: 34580310 PMC: 8476515. DOI: 10.1038/s41467-021-25992-8.

Trastuzumab immunogenicity development in patients' sera and in laboratory animals.

Kilany L, Gaber A, Aboulwafa M, Zedan H BMC Immunol. 2021; 22(1):15.

PMID: 33607941 PMC: 7893875. DOI: 10.1186/s12865-021-00405-z.

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

Jawa V, Terry F, Gokemeijer J, Mitra-Kaushik S, Roberts B, Tourdot S Front Immunol. 2020; 11:1301.

PMID: 32695107 PMC: 7338774. DOI: 10.3389/fimmu.2020.01301.

Structure-Based Immunogenicity Prediction of Uricase from Fungal (Aspergillus flavus), Bacterial (Bacillus subtillis) and Mammalian Sources Using Immunoinformatic Approach.

Tripathi S, Parmar J, Kumar A Protein J. 2020; 39(2):133-144.

PMID: 32221804 DOI: 10.1007/s10930-020-09886-0.