Self-reactive germline-like TCR alpha chains shared between blood and pancreas

Author:

Linsley Peter1ORCID,Nakayama Maki2,Balmas Elisa3,Chen Janice3,Pour Fariba3,Bansal Shubham3,Serti Elisavet4ORCID,Speake Cate3ORCID,Pugliese Alberto5,Cerosaletti Karen6ORCID

Affiliation:

1. Benaroya Research Institute at Virginia Mason

2. Barbara Davis Center for Childhood Diabetes

3. Benaroya Research Institute

4. The Henry Jackson Foundation

5. City of Hope

6. Benaroya Research Institute, Seattle, WA

Abstract

Abstract Human islet antigen reactive CD4 + memory T cells (IAR T cells) from peripheral blood have been studied extensively for their role in the pathogenesis of autoimmune type 1 diabetes (T1D). However, IAR T cells are rare, and it remains poorly understood how they affect T1D progression in the pancreas. Using single cell RNA-sequencing coupled with a multiplexed activation induced marker (AIM) enrichment assay, we identified paired TCR alpha/beta (TRA/TRB) T cell receptors (TCRs) in IAR T cells from the blood of healthy, at-risk, new onset, and established T1D donors. Using TCR sequences as barcodes, we measured infiltration of IAR T cells from blood into pancreas of organ donors with and without T1D. We detected extensive TCR sharing between IAR T cells from peripheral blood and pancreatic infiltrating T cells (PIT), with perfectly matched or single mismatched TRA junctions and J gene regions, comprising ~ 34% of unique IAR TCRs. PIT-matching IAR T cells had public TRA chains that showed increased use of germline-encoded residues in epitope engagement and a propensity for cross-reactivity. The link with T cells in the pancreas implicates autoreactive IAR T cells with shared TRA junctions and increased levels in blood with the prediabetic and new onset phases of T1D progression.

Publisher

Research Square Platform LLC

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