Targeting B Cells and Plasma Cells in Glomerular Disease.

IF 10.3 1区医学 Q1 UROLOGY & NEPHROLOGY

Journal of The American Society of Nephrology Pub Date : 2025-06-04 DOI:10.1681/ASN.0000000772

Syeda Behjat Ahmad, J Ashley Jefferson

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Abstract

Abstract: Loss of tolerance and the production of self-reactive autoantibodies by the humoral immune system are central to the pathogenesis of many glomerular diseases. These antibodies are produced by plasmablasts and plasma cells, the end-products of B cell lineage development within the bone marrow and secondary lymphoid tissues. In addition to antibody production, B cells also present antigen to T cells and produce pro-inflammatory cytokines. Non-targeted immunosuppression has shown efficacy in glomerular disease, but is associated with multiple side effects, and there remains a high proportion of patients with resistant disease. In this manuscript, we will review the biology of antibody secreting cells, and focus on therapeutics that specifically target B cells and plasma cells. We will review B cell depletion strategies, including anti-CD20 monoclonal antibodies, BAFF and APRIL inhibition and B cell receptor inhibition highlighting their role in different glomerular diseases and outline reasons for therapeutic resistance. We will also review plasma cell directed therapies including proteasome inhibition and anti-CD38 therapies, and discuss novel treatments including CAR-T therapy and bispecific T cell engagers.

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靶向B细胞和浆细胞在肾小球疾病中的作用

摘要：体液免疫系统的耐受性丧失和自身反应性抗体的产生是许多肾小球疾病发病机制的核心。这些抗体是由浆母细胞和浆细胞产生的，它们是骨髓和次级淋巴组织中B细胞谱系发育的最终产物。除了产生抗体外，B细胞还向T细胞呈递抗原并产生促炎细胞因子。非靶向免疫抑制在肾小球疾病中已显示出疗效，但与多重副作用相关，并且仍有高比例的患者出现耐药疾病。在这篇文章中，我们将回顾抗体分泌细胞的生物学，并重点介绍特异性靶向B细胞和浆细胞的治疗方法。我们将回顾B细胞耗竭策略，包括抗cd20单克隆抗体、BAFF和APRIL抑制以及B细胞受体抑制，强调它们在不同肾小球疾病中的作用，并概述治疗耐药的原因。我们还将回顾包括蛋白酶体抑制和抗cd38疗法在内的浆细胞定向疗法，并讨论包括CAR-T疗法和双特异性T细胞参与疗法在内的新疗法。

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来源期刊

Journal of The American Society of Nephrology 医学-泌尿学与肾脏学

CiteScore

22.40

自引率

2.90%

发文量

492

审稿时长

3-8 weeks

期刊介绍： The Journal of the American Society of Nephrology (JASN) stands as the preeminent kidney journal globally, offering an exceptional synthesis of cutting-edge basic research, clinical epidemiology, meta-analysis, and relevant editorial content. Representing a comprehensive resource, JASN encompasses clinical research, editorials distilling key findings, perspectives, and timely reviews. Editorials are skillfully crafted to elucidate the essential insights of the parent article, while JASN actively encourages the submission of Letters to the Editor discussing recently published articles. The reviews featured in JASN are consistently erudite and comprehensive, providing thorough coverage of respective fields. Since its inception in July 1990, JASN has been a monthly publication. JASN publishes original research reports and editorial content across a spectrum of basic and clinical science relevant to the broad discipline of nephrology. Topics covered include renal cell biology, developmental biology of the kidney, genetics of kidney disease, cell and transport physiology, hemodynamics and vascular regulation, mechanisms of blood pressure regulation, renal immunology, kidney pathology, pathophysiology of kidney diseases, nephrolithiasis, clinical nephrology (including dialysis and transplantation), and hypertension. Furthermore, articles addressing healthcare policy and care delivery issues relevant to nephrology are warmly welcomed.