Human anti-smallpox long-lived memory B cells are defined by dynamic interactions in the splenic niche and long-lasting germinal center imprinting

人类抗天花长寿命记忆B细胞的特征是脾脏微环境中的动态相互作用和持久的生发中心印记。

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作者:Pascal Chappert,François Huetz,Marie-Alix Espinasse,Fabrice Chatonnet,Louise Pannetier,Lucie Da Silva,Clara Goetz,Jérome Mégret,Aurélien Sokal,Etienne Crickx,Ivan Nemazanyy,Vincent Jung,Chiara Guerrera,Sébastien Storck,Matthieu Mahévas,Antonio Cosma,Patrick Revy,Thierry Fest,Claude-Agnès Reynaud,Jean-Claude Weill

Abstract

Memory B cells (MBCs) can persist for a lifetime, but the mechanisms that allow their long-term survival remain poorly understood. Here, we isolated and analyzed human splenic smallpox/vaccinia protein B5-specific MBCs in individuals who were vaccinated more than 40 years ago. Only a handful of clones persisted over such an extended period, and they displayed limited intra-clonal diversity with signs of extensive affinity-based selection. These long-lived MBCs appeared enriched in a CD21hiCD20hi IgG+ splenic B cell subset displaying a marginal-zone-like NOTCH/MYC-driven signature, but they did not harbor a unique longevity-associated transcriptional or metabolic profile. Finally, the telomeres of B5-specific, long-lived MBCs were longer than those in patient-paired naive B cells in all the samples analyzed. Overall, these results imply that separate mechanisms such as early telomere elongation, affinity selection during the contraction phase, and access to a specific niche contribute to ensuring the functional longevity of MBCs.

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