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Folding and Misfolding of Human Membrane Proteins in Health andDisease: From Single Molecules to Cellular Proteostasis

机译:人体健康中膜蛋白的折叠和错误折叠疾病:从单分子到细胞蛋白变性

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摘要

Advances over the past 25 years have revealed much about how the structural properties of membranes and associated proteins are linked to the thermodynamics and kinetics of membrane protein (MP) folding. At the same time biochemical progress has outlined how cellular proteostasis networks mediate MP folding and manage misfolding in the cell. When combined with results from genomic sequencing, these studies have established paradigms for how MP folding and misfolding are linked to the molecular etiologies of a variety of diseases. This emerging framework has paved the way for the development of a new class of small molecule “pharmacological chaperones” that bind to and stabilize misfolded MP variants, some of which are now in clinical use. In this review, we comprehensively outline current perspectives on the folding and misfolding of integral MPs as well as the mechanisms of cellular MP quality control. Based on these perspectives, we highlight new opportunities for innovations that bridge our molecular understanding of the energetics of MP folding with the nuanced complexity of biologicalsystems. Given the many linkages between MP misfolding and human disease,we also examine some of the exciting opportunities to leverage theseadvances to address emerging challenges in the development of therapeuticsand precision medicine.
机译:过去25年的进展揭示了膜和相关蛋白的结构特性如何与膜蛋白(MP)折叠的热力学和动力学联系在一起。同时,生物化学的进展概述了细胞变形蛋白网络如何介导MP折叠并管理细胞中的错误折叠。当与基因组测序的结果相结合时,这些研究就MP折叠和错折叠如何与多种疾病的分子病因学建立了联系。这一新兴框架为开发新型小分子“药理分子伴侣”铺平了道路,这些小分子“分子伴侣”可结合并稳定错误折叠的MP变体,其中一些现已投入临床使用。在这篇综述中,我们全面概述了有关MP折叠和错折叠以及细胞MP质量控制机制的当前观点。基于这些观点,我们强调了创新的新机遇,这些创新将我们对MP折叠能量学的分子理解与生物学的细微差别联系起来系统。鉴于MP错误折叠与人类疾病之间存在许多联系,我们还将研究利用这些机遇的一些令人兴奋的机会解决疗法发展中新挑战的进展和精密医学。

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