Xu Yue, Cui Lei, Dibello Anthony, Wang Lihui, Lee Juhyung, Saidi Layla, Lee Jin-Gu, Ye Yihong
Laboratory of Molecular Biology, National Institute of Diabetes and Digestive and Kidney Diseases, National Institutes of Health, Bethesda, MD 20892 USA.
Cell Discov. 2018 Mar 6;4:11. doi: 10.1038/s41421-018-0012-7. eCollection 2018.
Cell-to-cell transmission of misfolded proteins propagates proteotoxic stress in multicellular organisms when transmitted polypeptides serve as a seeding template to cause protein misfolding in recipient cells, but how misfolded proteins are released from cells to initiate this process is unclear. Misfolding-associated protein secretion (MAPS) is an unconventional protein-disposing mechanism that specifically exports misfolded cytosolic proteins including various neurodegenerative disease-causing proteins. Here we establish the HSC70 co-chaperone DNAJC5 as an essential mediator of MAPS. USP19, a previously uncovered MAPS regulator binds HSC70 and acts upstream of HSC70 and DNAJC5. We further show that as a membrane-associated protein localized preferentially to late endosomes and lysosomes, DNAJC5 can chaperone MAPS client proteins to the cell exterior. Intriguingly, upon secretion, misfolded proteins can be taken up through endocytosis and eventually degraded in the lysosome. Collectively, these findings suggest a transcellular protein quality control regulatory pathway in which a deubiquitinase-chaperone axis forms a "triaging hub", transferring aberrant polypeptides from stressed cells to healthy ones for disposal.
当错误折叠的蛋白质在细胞间传播时,多细胞生物中错误折叠的蛋白质的细胞间传播会引发蛋白毒性应激,因为传递的多肽充当种子模板,导致受体细胞中的蛋白质错误折叠,但错误折叠的蛋白质如何从细胞中释放以启动这一过程尚不清楚。错误折叠相关蛋白分泌(MAPS)是一种非常规的蛋白质处理机制,它特异性地输出错误折叠的胞质蛋白,包括各种导致神经退行性疾病的蛋白。在这里,我们确定热休克蛋白70(HSC70)的共伴侣蛋白DNAJC5是MAPS的关键介质。USP19是一种先前发现的MAPS调节剂,它与HSC70结合,并在HSC70和DNAJC5的上游起作用。我们进一步表明,作为一种优先定位于晚期内体和溶酶体的膜相关蛋白,DNAJC5可以将MAPS的客户蛋白伴侣到细胞外。有趣的是,在分泌后,错误折叠的蛋白质可以通过内吞作用被摄取,并最终在溶酶体中降解。总的来说,这些发现表明了一种跨细胞蛋白质质量控制调节途径,其中去泛素酶-伴侣轴形成一个“分类枢纽”,将异常多肽从应激细胞转移到健康细胞进行处理。
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