Immunity and Cancer, Francis Crick Institute, London, UK.
Retroviral Immunology, Francis Crick Institute, London, UK.
J Exp Med. 2020 Jul 6;217(7). doi: 10.1084/jem.20191933.
Memory B cells (MBCs) are key for protection from reinfection. However, it is mechanistically unclear how germinal center (GC) B cells differentiate into MBCs. MYC is transiently induced in cells fated for GC expansion and plasma cell (PC) formation, so-called positively selected GC B cells. We found that these cells coexpressed MYC and MIZ1 (MYC-interacting zinc-finger protein 1 [ZBTB17]). MYC and MIZ1 are transcriptional activators; however, they form a transcriptional repressor complex that represses MIZ1 target genes. Mice lacking MYC-MIZ1 complexes displayed impaired cell cycle entry of positively selected GC B cells and reduced GC B cell expansion and PC formation. Notably, absence of MYC-MIZ1 complexes in positively selected GC B cells led to a gene expression profile alike that of MBCs and increased MBC differentiation. Thus, at the GC positive selection stage, MYC-MIZ1 complexes are required for effective GC expansion and PC formation and to restrict MBC differentiation. We propose that MYC and MIZ1 form a module that regulates GC B cell fate.
记忆 B 细胞(MBC)是防止再次感染的关键。然而,生发中心(GC)B 细胞如何分化为 MBC 在机制上尚不清楚。在注定要进行 GC 扩增和浆细胞(PC)形成的细胞中,即所谓的阳性选择 GC B 细胞,MYC 会短暂诱导。我们发现这些细胞共表达 MYC 和 MIZ1(MYC 相互作用的锌指蛋白 1 [ZBTB17])。MYC 和 MIZ1 是转录激活物;然而,它们形成转录抑制复合物,抑制 MIZ1 靶基因。缺乏 MYC-MIZ1 复合物的小鼠显示阳性选择 GC B 细胞的细胞周期进入受损,GC B 细胞扩增和 PC 形成减少。值得注意的是,阳性选择 GC B 细胞中缺乏 MYC-MIZ1 复合物会导致类似于 MBC 的基因表达谱,并增加 MBC 分化。因此,在 GC 阳性选择阶段,MYC-MIZ1 复合物对于有效的 GC 扩增和 PC 形成以及限制 MBC 分化是必需的。我们提出,MYC 和 MIZ1 形成一个调节 GC B 细胞命运的模块。
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