Autoantibodies Against DNA Topoisomerase I Promote Renal Allograft Rejection by Increasing Alloreactive T Cell Responses

Overview

Journal Am J Transplant

Publisher Elsevier

Specialty General Surgery

Date 2023 Apr 21

PMID 37084848

Authors

Victoria Gorbacheva

Ran Fan

Satoshi Miyairi

Robert L Fairchild

William M Baldwin 3rd

Anna Valujskikh

Affiliations

Soon will be listed here.

Abstract

Antibodies reactive to self-antigens are an important component of posttransplant immune responses. The generation requirements and functions of autoantibodies, as well as the mechanisms of their influence on alloimmune responses, still remain to be determined. Our study investigated the contribution of autoimmunity during rejection of renal allografts. We have previously characterized a mouse model in which the acute rejection of a life-supporting kidney allograft is mediated by antibodies. At rejection, recipient sera screening against >4000 potential autoantigens revealed DNA topoisomerase I peptide 205-219 (TI-I) as the most prominent epitope. Subsequent analysis showed TI-I-reactive autoantibodies are induced in nonsensitized recipients of major histocompatibility complex-mismatched kidney allografts in a T cell-dependent manner. Immunization with TI-I broke self-tolerance, elicited TI-I immunoglobin G autoantibodies, and resulted in acute rejection of allogeneic but not syngeneic renal transplants. The graft loss was associated with increased priming of donor-reactive T cells but not with donor-specific alloantibodies elevation. Similarly, passive transfer of anti-TI-I sera following transplantation increased donor-reactive T cell activation with minimal effects on donor-specific alloantibody levels. The results identify DNA topoisomerase I as a novel self-antigen in transplant settings and demonstrate that autoantibodies enhance activation of donor-reactive T cells following renal transplantation.

Citing Articles

Marginal zone B cells are required for optimal humoral responses to allograft.

Gorbacheva V, Fan R, Gaudette B, Baldwin 3rd W, Fairchild R, Valujskikh A Am J Transplant. 2024; 25(1):48-59.

PMID: 39278625 PMC: 11734443. DOI: 10.1016/j.ajt.2024.09.004.

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