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细胞内蛋白质降解:从一个模糊的概念到溶酶体和泛素-蛋白酶体系统,再到人类疾病和药物靶向。

Intracellular protein degradation: from a vague idea through the lysosome and the ubiquitin-proteasome system and onto human diseases and drug targeting.

机构信息

Cancer and Vascular Biology Research Center, The Rappaport Faculty of Medicine and Research Institute, Technion-Israel Institute of Technology, Haifa, Israel.

出版信息

Neurodegener Dis. 2012;10(1-4):7-22. doi: 10.1159/000334283. Epub 2012 Feb 10.

Abstract

Between the 1950s and 1980s, scientists were focusing mostly on how the genetic code was transcribed to RNA and translated to proteins, but how proteins were degraded had remained a neglected research area. With the discovery of the lysosome by Christian de Duve it was assumed that cellular proteins are degraded within this organelle. Yet, several independent lines of experimental evidence strongly suggested that intracellular proteolysis was largely nonlysosomal, but the mechanisms involved have remained obscure. The discovery of the ubiquitin-proteasome system resolved the enigma. We now recognize that degradation of intracellular proteins is involved in the regulation of a broad array of cellular processes, such as cell cycle and division, regulation of transcription factors, and assurance of the cellular quality control. Not surprisingly, aberrations in the system have been implicated in the pathogenesis of human disease, such as malignancies and neurodegenerative disorders, which subsequently led to an increasing effort to develop mechanism-based drugs.

摘要

在 20 世纪 50 年代至 80 年代期间,科学家们主要关注的是遗传密码如何转录为 RNA 并翻译成蛋白质,但蛋白质的降解过程一直是一个被忽视的研究领域。随着克里斯蒂安·德迪夫(Christian de Duve)发现溶酶体,人们曾假设细胞内的蛋白质在这个细胞器内被降解。然而,几条独立的实验证据线强烈表明,细胞内的蛋白水解作用在很大程度上是非溶酶体的,但相关的机制仍然不清楚。泛素-蛋白酶体系统的发现解决了这个谜团。我们现在认识到,细胞内蛋白质的降解参与了广泛的细胞过程的调节,如细胞周期和分裂、转录因子的调节以及细胞质量控制的保证。毫不奇怪,该系统的异常与人类疾病的发病机制有关,如恶性肿瘤和神经退行性疾病,这随后导致了越来越多的努力来开发基于机制的药物。

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