Autoreactive T Cell Receptors with Shared Germline-like α Chains in Type 1 Diabetes

Overview

Journal JCI Insight

Specialties Biomedical Engineering
General Medicine

Date 2021 Nov 22

PMID 34806648

Citations 15

Authors

Peter S Linsley

Fariba Barahmand-Pour-Whitman

Elisa Balmas

Hannah A DeBerg

Kaitlin J Flynn

Alex K Hu

Mario G Rosasco

Janice Chen

Colin ORourke

Elisavet Serti

Vivian H Gersuk

Keshav Motwani

Howard R Seay

Todd M Brusko

William W Kwok

Cate Speake

Carla J Greenbaum

Gerald T Nepom

Karen Cerosaletti

Affiliations

Soon will be listed here.

Abstract

Human islet antigen reactive CD4+ memory T cells (IAR T cells) play a key role in the pathogenesis of autoimmune type 1 diabetes (T1D). Using single-cell RNA sequencing (scRNA-Seq) to identify T cell receptors (TCRs) in IAR T cells, we have identified a class of TCRs that share TCRα chains between individuals ("public" chains). We isolated IAR T cells from blood of healthy, new-onset T1D and established T1D donors using multiplexed CD154 enrichment and identified paired TCRαβ sequences from 2767 individual cells. More than a quarter of cells shared TCR junctions between 2 or more cells ("expanded"), and 29/47 (~62%) of expanded TCRs tested showed specificity for islet antigen epitopes. Public TCRs sharing TCRα junctions were most prominent in new-onset T1D. Public TCR sequences were more germline like than expanded unique, or "private," TCRs, and had shorter junction sequences, suggestive of fewer random nucleotide insertions. Public TCRα junctions were often paired with mismatched TCRβ junctions in TCRs; remarkably, a subset of these TCRs exhibited cross-reactivity toward distinct islet antigen peptides. Our findings demonstrate a prevalent population of IAR T cells with diverse specificities determined by TCRs with restricted TCRα junctions and germline-constrained antigen recognition properties. Since these "innate-like" TCRs differ from previously described immunodominant TCRβ chains in autoimmunity, they have implications for fundamental studies of disease mechanisms. Self-reactive restricted TCRα chains and their associated epitopes should be considered in fundamental and translational investigations of TCRs in T1D.

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