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Transplantation tolerance modifies donor-specific B cell fate to suppress de novo alloreactive B cells.


ABSTRACT: The absence of alloantibodies is a feature of transplantation tolerance. Although the lack of T cell help has been evoked to explain this absence, herein we provide evidence for B cell-intrinsic tolerance mechanisms. Using a murine model of heart tolerance, we showed that alloreactive B cells were not deleted but rapidly lost their ability to differentiate into germinal center B cells and secrete donor-specific antibodies. We inferred that tolerant alloreactive B cells retained their ability to sense alloantigen because they continued to drive T cell maturation into CXCR5+PD-1+ T follicular helper cells. Unexpectedly, dysfunctional alloreactive B cells acquired the ability to inhibit antibody production by new naive B cells in an antigen-specific manner. Thus, tolerant alloreactive B cells contribute to transplantation tolerance by foregoing germinal center responses while retaining their ability to function as antigen-presenting cells and by actively suppressing de novo alloreactive B cell responses.

SUBMITTER: Khiew SH 

PROVIDER: S-EPMC7329196 | biostudies-literature | 2020 Jul

REPOSITORIES: biostudies-literature

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Transplantation tolerance modifies donor-specific B cell fate to suppress de novo alloreactive B cells.

Khiew Stella Hw SH   Jain Dharmendra D   Chen Jianjun J   Yang Jinghui J   Yin Dengping D   Young James S JS   Dent Alexander A   Sciammas Roger R   Alegre Maria-Luisa ML   Chong Anita S AS  

The Journal of clinical investigation 20200701 7


The absence of alloantibodies is a feature of transplantation tolerance. Although the lack of T cell help has been evoked to explain this absence, herein we provide evidence for B cell-intrinsic tolerance mechanisms. Using a murine model of heart tolerance, we showed that alloreactive B cells were not deleted but rapidly lost their ability to differentiate into germinal center B cells and secrete donor-specific antibodies. We inferred that tolerant alloreactive B cells retained their ability to  ...[more]

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