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非分泌性B细胞中快速的B细胞受体诱导的未折叠蛋白反应与促凋亡和抗凋亡细胞命运相关。

Rapid B cell receptor-induced unfolded protein response in nonsecretory B cells correlates with pro- versus antiapoptotic cell fate.

作者信息

Skalet Alison H, Isler Jennifer A, King Leslie B, Harding Heather P, Ron David, Monroe John G

机构信息

Department of Pathology and Laboratory Medicine, University of Pennsylvania School of Medicine, Philadelphia, Pennsylvania 19104, USA.

出版信息

J Biol Chem. 2005 Dec 2;280(48):39762-71. doi: 10.1074/jbc.M502640200. Epub 2005 Sep 27.

Abstract

The adaptive unfolded protein response (UPR) is essential for the development of antibody-secreting plasma cells. B cells induced by lipopolysaccharide (LPS) to differentiate into plasma cells exhibit a nonclassical UPR reported to anticipate endoplasmic reticulum stress prior to immunoglobulin production. Here we demonstrate that activation of a physiologic UPR is not limited to cells undergoing secretory cell differentiation. We identify B cell receptor (BCR) signaling as an unexpected physiologic UPR trigger and demonstrate that in mature B cells, BCR stimulation induces a short lived UPR similar to the LPS-triggered nonclassical UPR. However, unlike LPS, BCR stimulation does not induce plasma cell differentiation. Furthermore, the BCR-induced UPR is not limited to cells in which BCR induces activation, since a UPR is also induced in transitional immature B cells that respond to BCR stimulation with a rapid apoptotic fate. This response involves sustained up-regulation of Chop mRNA indicative of a terminal UPR. Whereas sustained Chop expression correlates with the ultimate fate of the BCR-triggered B cell and not its developmental stage, Chop-/- B cells undergo apoptosis, indicating that CHOP is not required for this process. These studies establish a system whereby a terminal or adaptive UPR can be alternatively triggered by physiologic stimuli.

摘要

适应性未折叠蛋白反应(UPR)对于分泌抗体的浆细胞的发育至关重要。由脂多糖(LPS)诱导分化为浆细胞的B细胞表现出一种非经典的UPR,据报道这种UPR在免疫球蛋白产生之前就可预测内质网应激。在此,我们证明生理性UPR的激活并不局限于经历分泌细胞分化的细胞。我们确定B细胞受体(BCR)信号传导是一种意想不到的生理性UPR触发因素,并证明在成熟B细胞中,BCR刺激会诱导一种类似于LPS触发的非经典UPR的短暂UPR。然而,与LPS不同,BCR刺激不会诱导浆细胞分化。此外,BCR诱导的UPR并不局限于BCR诱导激活的细胞,因为在对BCR刺激产生快速凋亡命运反应的过渡性未成熟B细胞中也会诱导UPR。这种反应涉及Chop mRNA的持续上调,表明是一种终末UPR。虽然持续的Chop表达与BCR触发的B细胞的最终命运相关,而与其发育阶段无关,但Chop基因敲除的B细胞会发生凋亡,这表明CHOP对于此过程并非必需。这些研究建立了一个系统,通过该系统终末或适应性UPR可由生理性刺激交替触发。

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