Germinal center (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, combining imaging, molecular, and genomic approaches, we defined 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 GCs in the salivary glands of Sjögren's disease, defining its role in autoimmunity.
Autophagy is an upstream mediator of chromatin dynamics in normal and autoimmune germinal center B cells.
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作者:Sallan Marta C, Filipsky Filip, Shi Christina H, Pontarini Elena, Terranova-Barberio Manuela, Beattie Gordon, Clear Andrew, Bombardieri Michele, Yip Kevin Y, Calado Dinis Pedro, Cragg Mark S, James Sonya, Carter Mathew, Okosun Jessica, Gribben John G, Klymenko Tanya, Braun Andrejs
期刊: | Journal of Clinical Investigation | 影响因子: | 13.600 |
时间: | 2025 | 起止号: | 2025 May 15; 135(13):e178920 |
doi: | 10.1172/JCI178920 |
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