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Properties of regulatory B cells regulating B cell targets.


ABSTRACT: Regulatory B cells (Bregs) have shown promise as anti-rejection therapy applied to organ transplantation. However, less is known about their effect on other B cell populations that are involved in chronic graft rejection. We recently uncovered that naïve B cells, stimulated by TLR ligand agonists, converted into B cells with regulatory properties (Bregs-TLR) that prevented allograft rejection. Here, we examine the granular phenotype and regulatory properties of Breg-TLR cells suppressing B cells. Cocultures of Bregs-TLR with LPS-activated B cells showed a dose-dependent suppression of targeted B cell proliferation. Adoptive transfers of Bregs-TLR induced a decline in antibody responses to antigenically disparate skin grafts. The role of Breg BCR specificity in regulation was assessed using B cell-deficient mice replenished with transgenic BCR (OB1) and TCR (OT-II) lymphocytes of matching antigenic specificity. Results indicated that proliferation of OB1 B cells, mediated through help from CD4+ OT-II cells, was suppressed by OB1 Bregs of similar specificity. Transcriptomic analyses indicated that Bregs-TLR suppression is associated with a block in targeted B cell differentiation controlled by PRDM1 (Blimp1). This work uncovered the regulatory properties of a new brand of Breg cells and provided mechanistic insights into potential applications of Breg therapy in transplantation.

SUBMITTER: Fu Q 

PROVIDER: S-EPMC8639638 | biostudies-literature | 2021 Dec

REPOSITORIES: biostudies-literature

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Properties of regulatory B cells regulating B cell targets.

Fu Qiang Q   Lee Kang Mi KM   Huai Guoli G   Deng Kevin K   Agarwal Divyansh D   Rickert Charles G CG   Feeney Noel N   Matheson Rudy R   Yang Hongji H   LeGuern Christian C   Deng Shaoping S   Markmann James F JF  

American journal of transplantation : official journal of the American Society of Transplantation and the American Society of Transplant Surgeons 20210906 12


Regulatory B cells (Bregs) have shown promise as anti-rejection therapy applied to organ transplantation. However, less is known about their effect on other B cell populations that are involved in chronic graft rejection. We recently uncovered that naïve B cells, stimulated by TLR ligand agonists, converted into B cells with regulatory properties (Bregs-TLR) that prevented allograft rejection. Here, we examine the granular phenotype and regulatory properties of Breg-TLR cells suppressing B cells  ...[more]

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