一个依赖于血栓反应蛋白的内质网应激保护反应途径。
A thrombospondin-dependent pathway for a protective ER stress response.
机构信息
Department of Pediatrics, Cincinnati Children's Hospital, University of Cincinnati, OH 45247, USA.
出版信息
Cell. 2012 Jun 8;149(6):1257-68. doi: 10.1016/j.cell.2012.03.050.
Abstract
Thrombospondin (Thbs) proteins are induced in sites of tissue damage or active remodeling. The endoplasmic reticulum (ER) stress response is also prominently induced with disease where it regulates protein production and resolution of misfolded proteins. Here we describe a function for Thbs as ER-resident effectors of an adaptive ER stress response. Thbs4 cardiac-specific transgenic mice were protected from myocardial injury, whereas Thbs4(-/-) mice were sensitized to cardiac maladaptation. Thbs induction produced a unique profile of adaptive ER stress response factors and expansion of the ER and downstream vesicles. Thbs bind the ER lumenal domain of activating transcription factor 6α (Atf6α) to promote its nuclear shuttling. Thbs4(-/-) mice showed blunted activation of Atf6α and other ER stress-response factors with injury, and Thbs4-mediated protection was lost upon Atf6α deletion. Hence, Thbs can function inside the cell during disease remodeling to augment ER function and protect through a mechanism involving regulation of Atf6α.
摘要
血栓反应蛋白(Thbs)蛋白在组织损伤或活跃重塑部位被诱导产生。内质网(ER)应激反应也在疾病中明显被诱导,它调节蛋白质的产生和错误折叠蛋白质的解决。在这里,我们描述了 Thbs 作为内质网驻留效应物的适应性 ER 应激反应的功能。Thbs4 心脏特异性转基因小鼠对心肌损伤有保护作用,而 Thbs4(-/-) 小鼠对心脏适应不良敏感。Thbs 的诱导产生了适应性 ER 应激反应因子的独特谱,并扩展了内质网和下游小泡。Thbs 与激活转录因子 6α(Atf6α)的内质网腔域结合,以促进其核穿梭。在损伤时,Thbs4(-/-) 小鼠中 Atf6α 和其他 ER 应激反应因子的激活减弱,而在 Atf6α 缺失时,Thbs4 介导的保护作用丧失。因此,在疾病重塑过程中,Thbs 可以在细胞内发挥作用,增强 ER 功能,并通过涉及调节 Atf6α的机制来保护。
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