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Memory B Cells of Mice and Humans
Annual Review of Immunology ( IF 29.7 ) Pub Date : 2017-04-26 00:00:00 , DOI: 10.1146/annurev-immunol-041015-055531
Florian Weisel 1 , Mark Shlomchik 1
Affiliation  

We comprehensively review memory B cells (MBCs), covering the definition of MBCs and their identities and subsets, how MBCs are generated, where they are localized, how they are maintained, and how they are reactivated. Whereas naive B cells adopt multiple fates upon stimulation, MBCs are more restricted in their responses. Evolving work reveals that the MBC compartment in mice and humans consists of distinct subpopulations with differing effector functions. We discuss the various approaches to define subsets and subset-specific roles. A major theme is the need to both deliver faster effector function upon reexposure and readapt to antigenically variant pathogens while avoiding burnout, which would be the result if all MBCs generated only terminal effector function. We discuss cell-intrinsic differences in gene expression and signaling that underlie differences in function between MBCs and naive B cells and among MBC subsets and how this leads to memory responses.

中文翻译:


小鼠和人类的记忆B细胞

我们全面回顾了记忆B细胞(MBC),涵盖了MBC的定义及其身份和子集,MBC的生成方式,它们的定位位置,如何维护以及如何重新激活它们。幼稚的B细胞在刺激时具有多种命运,而MBC的反应受到更多限制。不断发展的研究表明,小鼠和人的MBC区室由具有不同效应子功能的不同亚群组成。我们讨论了定义子集和特定于子集的角色的各种方法。一个主要主题是既需要在重新暴露时提供更快的效应子功能,又需要重新适应抗原性变异病原体,同时避免倦怠,这是如果所有MBC仅产生末端效应子功能的结果。

更新日期:2017-04-26
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