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Proteostatic Tactics in the Strategy of Sterol Regulation

机译:甾醇调节策略中的蛋白质策略

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In eukaryotes, the synthesis and uptake of sterols undergo stringent multivalent regulation. Both individual enzymes and transcriptional networks are controlled to meet changing needs of the many sterol pathway products. Regulation is tailored by evolution to match regulatory constraints, which can be very different in distinct species. Nevertheless, a broadly conserved feature of many aspects of sterol regulation is employment of proteostasis mechanisms to bring about control of individual proteins. Proteostasis is the set of processes that maintain homeostasis of a dynamic proteome. Proteostasis includes protein quality control pathways for the detection, and then the correction or destruction, of the many misfolded proteins that arise as an unavoidable feature of protein-based life. Protein quality control displays not only the remarkable breadth needed to manage the wide variety of client molecules, but also extreme specificity toward the misfolded variants of a given protein. These features are amenable to evolutionary usurpation as a means to regulate proteins, and this approach has been used in sterol regulation. We describe both well-trod and less familiar versions of the interface between proteostasis and sterol regulation and suggest some underlying ideas with broad biological and clinical applicability.
机译:在真核生物中,甾醇的合成和摄取经历严格的多价调节。控制各种酶和转录网络,以满足许多甾醇途径产品的不断变化的需求。通过进化来定制规范以匹配调节限制,这可能在不同的物种中非常不同。尽管如此,甾醇调节许多方面的广泛节省特征是蛋白质棘上机制的就业,以实现单个蛋白质的控制。蛋白质是维持动态蛋白质组的稳态的一组过程。蛋白质抑制型包括用于检测的蛋白质质量控​​制途径,然后是校正或破坏的许多错误蛋白质,其作为蛋白质寿命的不可避免的特征。蛋白质质量控​​制不仅显示了管理各种客户分子所需的显着宽度,而且朝着给定蛋白质的错误折叠变体的极端特异性。这些特征适用于进化的usurpation作为调节蛋白质的手段,并且这种方法已用于甾醇调节。我们描述了蛋白质和甾醇调节之间的界面良好的良好熟悉的界面,并提出了具有广泛生物学和临床适用性的潜在思路。

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