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Blimp-1 controls plasma cell function through the regulation of immunoglobulin secretion and the unfolded protein response

机译:Blimp-1通过调节免疫球蛋白分泌和未折叠的蛋白质反应来控制浆细胞功能

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Plasma cell differentiation requires silencing of B cell transcription, while it establishes antibody-secretory function and long-term survival. The transcription factors Blimp-1 and IRF4 are essential for the generation of plasma cells; however, their function in mature plasma cells has remained elusive. We found that while IRF4 was essential for the survival of plasma cells, Blimp-1 was dispensable for this. Blimp-l-deficient plasma cells retained their transcriptional identity but lost the ability to secrete antibody. Blimp-1 regulated many components of the unfolded protein response (UPR), including XBP-1 and ATF6. The overlap in the functions of Blimp-1 and XBP-1 was restricted to that response, with Blimp-1 uniquely regulating activity of the kinase mTOR and the size of plasma cells. Thus, Blimp-1 was required for the unique physiological ability of plasma cells that enables the secretion of protective antibody.
机译:浆细胞分化需要沉默B细胞转录,同时建立抗体分泌功能和长期存活。转录因子Blimp-1和IRF4对于浆细胞的产生是必不可少的。然而,它们在成熟浆细胞中的功能仍然难以捉摸。我们发现,尽管IRF4对于浆细胞的生存至关重要,但Blimp-1却是不可缺少的。 Blimp-1缺陷型浆细胞保留了其转录同一性,但失去了分泌抗体的能力。 Blimp-1调节未折叠蛋白应答(UPR)的许多成分,包括XBP-1和ATF6。 Blimp-1和XBP-1在功能上的重叠仅限于该反应,而Blimp-1可以唯一调节激酶mTOR的活性和浆细胞的大小。因此,Blimp-1是浆细胞独特的生理功能所必需的,该功能能够分泌保护性抗体。

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