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Increased expression and retention of the secretory chaperone proSAAS following cell stress

机译:在细胞应激后增加分泌伴侣口腔的表达和保留

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The secretory pathway of neurons and endocrine cells contains a variety of mechanisms designed to combat cellular stress. These include not only the unfolded protein response pathways but also diverse chaperone proteins that collectively work to ensure proteostatic control of secreted and membrane-bound molecules. One of the least studied of these chaperones is the neural- and endocrine-specific molecule known as proSAAS. This small chaperone protein acts as a potent anti-aggregant both in vitro and in cellulo and also represents a cerebrospinal fluid biomarker in Alzheimer’s disease. In the present study, we have examined the idea that proSAAS, like other secretory chaperones, might represent a stress-responsive protein. We find that exposure of neural and endocrine cells to the cell stressors tunicamycin and thapsigargin increases cellular proSAAS mRNA and protein in Neuro2A cells. Paradoxically, proSAAS secretion is inhibited by these same drugs. Exposure of Neuro2A cells to low concentrations of the hypoxic stress inducer cobalt chloride, or to sodium arsenite, an oxidative stressor, also increases cellular proSAAS content and reduces its secretion. We conclude that the cellular levels of the small secretory chaperone proSAAS are positively modulated by cell stress.
机译:神经元和内分泌细胞的分泌途径含有各种旨在用于打击细胞应激的机制。这些不仅包括展开的蛋白质反应途径,而且包括各种伴侣蛋白,其共同作用,以确保分泌细胞和膜结合分子的突出控制。这些伴侣的最少研究之一是称为prosaas的神经和内分泌特异性分子。该小伴侣蛋白在体外和纤维素中起到有效的抗聚集作用,并且还代表阿尔茨海默病的脑脊液生物标志物。在本研究中,我们研究了像其他分泌伴侣一样的波特拉斯可能代表压力响应蛋白质的想法。我们发现,神经和内分泌细胞暴露于细胞压力源unicicamycin和Thapsigargin增加了神经部米细胞中的细胞前景mRNA和蛋白质。矛盾的是,这些相同的药物抑制了prosaas分泌物。 Neuro2a细胞暴露于低浓度的低氧应激诱导钴氯化钴,或氧化氧化胁迫频率,也增加了细胞前氧化含量并降低了其分泌。我们得出结论,小型分泌伴侣波纹的细胞水平通过细胞应力呈正地调节。

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