自噬是正常和自身免疫生发中心B细胞染色质动力学的上游介质。

Marta C Sallan,Filip Filipsky,Christina H Shi,Elena Pontarini,Manuela Terranova-Barberio,Gordon Beattie,Andrew Clear,Michele Bombardieri,Kevin Y Yip,Dinis Parente Calado,Mark S Cragg,Sonya James,Matthew J Carter,Jessica Okosun,John G Gribben,Tanya Klymenko,Andrejs Braun
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引用次数: 0

摘要

生发中心(GC) B细胞在维持抗体自身耐受性的同时,在建立强大的体液免疫反应和长期血清学免疫中起着关键作用。GC B细胞依靠自噬来提供抗原和维持体内平衡。然而,这些功能主要与光区相关,并不能解释GCs暗区自噬的时空上调。在这里,我们定义了一种控制GC B细胞在暗区过渡期间染色质可及性的功能机制。该机制将自噬和核Lamin B1动力学与其下游效应联系起来,包括体细胞超突变和抗体亲和成熟。此外,自噬-层粘连蛋白B1轴在干燥病唾液腺异常异位生发中心高度活跃,确定其在自身免疫中的作用。
本文章由计算机程序翻译,如有差异,请以英文原文为准。
Autophagy is an upstream mediator of chromatin dynamics in normal and autoimmune germinal centre B cells.
Germinal centre (GC) B cells are pivotal in establishing a robust humoral immune response and long-term serological immunity while maintaining antibody self-tolerance. GC B cells rely on autophagy for antigen presentation and homeostatic maintenance. However, these functions, primarily associated with the light zone, cannot explain the spatiotemporal autophagy upregulation in the dark zone of GCs. Here, we define a functional mechanism controlling chromatin accessibility in GC B cells during their dark zone transition. This mechanism links autophagy and nuclear Lamin B1 dynamics with their downstream effects, including somatic hypermutation and antibody affinity maturation. Moreover, the autophagy-Lamin B1 axis is highly active in the aberrant ectopic germinal centres in the salivary glands of Sjogren's disease, defining its role in autoimmunity.
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