B cell and antibody targeting of transplant alloantigen epitopes is supported by both self and allo-recognition

Author:

Killian John T.ORCID,King R. Glenn,Kizziah James L.,Fucile Christopher F.,Diaz-Avalos Ruben,Qiu Shihong,Silva-Sanchez Aaron,Mousseau Betty J.,Macon Kevin J.,Callahan Amanda R.,Yang Guang,Hossain M. Emon,Akther Jobaida,Good Daryl B.,Kelso Susan,Houp Julie A.,Rosenblum Frida,Porrett Paige M.,Ong Song C.,Kumar Vineeta,Saphire Erica Ollmann,Kearney John F.,Randall Troy D.,Rosenberg Alexander F.,Green Todd J.,Lund Frances E.

Abstract

ABSTRACTDonor-specific antibody (DSA) responses against human leukocyte antigen (HLA) proteins mismatched between kidney transplant donors and recipients cause allograft loss. Using single-cell, molecular, structural, and proteomic techniques, we profiled the HLA-specific (alloreactive) B cell response in kidney and blood of a transplant recipient with antibody-mediated rejection (AMR). We identified 14 distinct alloreactive B cell lineages, which spanned the rejected organ and blood and expressed high-affinity anti-donor HLA-specific B cell receptors – many of which were clonally linked to circulating DSA. The alloreactive B cell response was focused on exposed, solvent-accessible mismatched HLA residues, while also demonstrating extensive contacts with self-HLA residues. Consistent with structural evidence of self-recognition, measurable self-reactivity by donor-specific B cells was common and positively correlated with anti-donor affinity maturation. Thus, allo- and self-reactive signatures appeared to converge, suggesting that during AMR, the recognition of non-self and breaches of tolerance conspire to produce a pathogenic donor-specific adaptive response.

Publisher

Cold Spring Harbor Laboratory

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