移植中的B细胞耐受性：免疫组库重塑是答案吗？

B-cell tolerance in transplantation: is repertoire remodeling the answer?

作者信息

Parsons Ronald F, Vivek Kumar, Redfield Robert R, Migone Thi-Sau, Cancro Michael P, Naji Ali, Noorchashm Hooman

机构信息

329 Stemmler Hall, 36th and Hamilton Walk, University of Pennsylvania School of Medicine, Harrison Department of Surgical Research, Philadelphia, PA 19104, USA, Tel.: +1 215 400 1806.

出版信息

Expert Rev Clin Immunol. 2009 Nov;5(6):703. doi: 10.1586/eci.09.63.

DOI:10.1586/eci.09.63

PMID:20161663

原文链接:https://pmc.ncbi.nlm.nih.gov/articles/PMC2819040/

Abstract

T lymphocytes are the primary targets of immunotherapy in clinical transplantation; however, B lymphocytes and their secreted alloantibodies are also highly detrimental to the allograft. Therefore, the achievement of sustained organ transplant survival will likely require the induction of B-lymphocyte tolerance. During development, acquisition of B-cell tolerance to self-antigens relies on clonal deletion in the early stages of B-cell compartment ontogeny. We contend that this mechanism should be recapitulated in the setting of alloantigens and organ transplantation to eliminate the alloreactive B-cell subset from the recipient. Clinically feasible targets of B-cell-directed immunotherapy, such as CD20 and B-lymphocyte stimulator (BLyS), should drive upcoming clinical trials aimed at remodeling the recipient B-cell repertoire.

摘要

T淋巴细胞是临床移植中免疫治疗的主要靶点；然而，B淋巴细胞及其分泌的同种异体抗体对同种异体移植物也有极大损害。因此，要实现器官移植的长期存活可能需要诱导B淋巴细胞耐受。在发育过程中，B细胞对自身抗原的耐受性获得依赖于B细胞区室个体发生早期阶段的克隆清除。我们认为，在同种异体抗原和器官移植的背景下应重现这一机制，以从受体中消除同种异体反应性B细胞亚群。针对B细胞的免疫治疗在临床上可行的靶点，如CD20和B淋巴细胞刺激因子（BLyS），应推动即将开展的旨在重塑受体B细胞库的临床试验。

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