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蛋白酶体:古菌视角

Proteasomes: perspectives from the Archaea.

作者信息

Maupin-Furlow Julie A, Gil Malgorzata A, Karadzic Ivanka M, Kirkland Phillip A, Reuter Christopher J

机构信息

Department of Microbiology and Cell Science, University of Florida, Gainesville, FL 32611-0700, USA.

出版信息

Front Biosci. 2004 May 1;9:1743-58. doi: 10.2741/1363.

Abstract

The development of whole systems approaches to microbiology (e.g. genomics and proteomics) has facilitated a global view of archaeal physiology. Surprisingly, as archaea respond to environmental signals, the majority of protein concentration changes that occur are not reflected at the mRNA level. This incongruity highlights the importance of post-transcription control mechanisms in these organisms. One of the central players in proteolysis is the proteasome, a multicatalytic energy-dependent protease. Proteasomes serve both proteolytic and non-proteolytic roles in protein quality control and in the regulation of cell function. The proteolytic active sites of these enzymes are housed within a central chamber of an elaborate nanocompartment termed the 20S proteasome or core particle. Axial gates, positioned at each end of this particle, restrict the type of substrate that can access the proteolytic active sites. Assortments of regulatory AAA complexes are predicted to recognize/bind and unfold substrate proteins, open the axial gates, and translocate substrate into the 20S core particle.

摘要

微生物学全系统方法(如基因组学和蛋白质组学)的发展促进了对古菌生理学的全局认识。令人惊讶的是,当古菌对环境信号作出反应时,发生的大多数蛋白质浓度变化并未在mRNA水平上体现出来。这种不一致凸显了转录后控制机制在这些生物体中的重要性。蛋白酶体是蛋白水解过程中的核心参与者之一,它是一种多催化的能量依赖性蛋白酶。蛋白酶体在蛋白质质量控制和细胞功能调节中发挥蛋白水解和非蛋白水解作用。这些酶的蛋白水解活性位点位于一个称为20S蛋白酶体或核心颗粒的精细纳米隔室的中央腔室内。位于该颗粒两端的轴向门限制了能够进入蛋白水解活性位点的底物类型。预计各种调节性AAA复合物可识别/结合并展开底物蛋白,打开轴向门,并将底物转运到20S核心颗粒中。

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