Arid1a-dependent canonical BAF complex suppresses inflammatory programs to drive efficient germinal center B cell responses

The mammalian Brg1/Brm-associated factor (BAF) complexes are major regulators of nucleosomal remodeling that are commonly mutated in several cancers, including germinal center (GC)-derived B cell lymphomas. However, the specific roles of different BAF complexes in GC B cell biology are not well unde...

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Veröffentlicht in:Nature immunology 2024-09, Vol.25 (9), p.1704-1717
Hauptverfasser: Abraham, Ajay, Samaniego-Castruita, Daniela, Han, Isabella, Ramesh, Prathyaya, Tran, Mi Thao, Paladino, Jillian, Kligfeld, Heather, Morgan, Roxroy C., Schmitz, Rebecca L., Southern, Rebecca M., Shukla, Ashima, Shukla, Vipul
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Sprache:eng
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Zusammenfassung:The mammalian Brg1/Brm-associated factor (BAF) complexes are major regulators of nucleosomal remodeling that are commonly mutated in several cancers, including germinal center (GC)-derived B cell lymphomas. However, the specific roles of different BAF complexes in GC B cell biology are not well understood. Here we show that the AT-rich interaction domain 1a (Arid1a) containing canonical BAF (cBAF) complex is required for maintenance of GCs and high-affinity antibody responses. While Arid1a-deficient B cells undergo initial activation, they fail to sustain the GC program. Arid1a establishes permissive chromatin landscapes for B cell activation and is concomitantly required to suppress inflammatory gene programs. The inflammatory signatures instigated by Arid1a deficiency promoted the recruitment of neutrophils and inflammatory monocytes. Dampening of inflammatory cues through interleukin-1β blockade or glucocorticoid receptor agonist partially rescued Arid1a-deficient GCs, highlighting a critical role for inflammation in impeding GCs. Our work reveals essential functions of Arid1a-dependent cBAF in promoting efficient GC responses. Shukla and colleagues show that the Arid1a-dependent BAF chromatin remodeling complex is required to maintain germinal center B cell programs.
ISSN:1529-2908
1529-2916
1529-2916
DOI:10.1038/s41590-024-01920-y