Hidden in Plain View: Discovery of Chimeric Diabetogenic CD4 T Cell Neo-Epitopes

Overview

Journal Front Immunol

Specialty Allergy & Immunology

Date 2021 May 14

PMID 33986758

Citations 2

Authors

Brendan K Reed

John W Kappler

Affiliations

Soon will be listed here.

Abstract

The T cell antigens driving autoimmune Type 1 Diabetes (T1D) have been pursued for more than three decades. When diabetogenic CD4 T cell clones and their relevant MHCII antigen presenting alleles were first identified in rodents and humans, the path to discovering the peptide epitopes within pancreatic beta cell proteins seemed straightforward. However, as experimental results accumulated, definitive data were often absent or controversial. Work within the last decade has helped to clear up some of the controversy by demonstrating that a number of the important MHCII presented epitopes are not encoded in the natural beta cell proteins, but in fact are fusions between peptide fragments derived from the same or different proteins. Recently, the mechanism for generating these MHCII diabetogenic chimeric epitopes has been attributed to a form of reverse proteolysis, called transpeptidation, a process that has been well-documented in the production of MHCI presented epitopes. In this mini-review we summarize these data and their implications for T1D and other autoimmune responses.

Citing Articles

Pathogenesis of Type 1 Diabetes: Established Facts and New Insights.

Zajec A, Trebusak Podkrajsek K, Tesovnik T, Sket R, cugalj Kern B, Jenko Bizjan B Genes (Basel). 2022; 13(4).

PMID: 35456512 PMC: 9032728. DOI: 10.3390/genes13040706.

Activation pathways that drive CD4 T cells to break tolerance in autoimmune diseases.

Krovi S, Kuchroo V Immunol Rev. 2022; 307(1):161-190.

PMID: 35142369 PMC: 9255211. DOI: 10.1111/imr.13071.

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