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因子促进核糖体组装的最新进展。

Recent developments in factor-facilitated ribosome assembly.

作者信息

Maki Jennifer A, Culver Gloria M

机构信息

Department of Biochemistry, Biophysics and Molecular Biology, Iowa State University, Ames, IA 50011, USA.

出版信息

Methods. 2005 Jul;36(3):313-20. doi: 10.1016/j.ymeth.2005.04.008.

Abstract

Escherichia coli ribosomal subunits can be reconstituted in vitro under highly optimized conditions. These reconstitution systems have proven invaluable for the study of ribosomal subunit assembly. While E. coli ribosomal subunits can self-assemble in vitro there has been much speculation regarding the existence of extra-ribosomal assembly factors that act in functional subunit formation in vivo. Recently, a biochemical assay has been implemented to identify factors that facilitate a single, critical step in 30S subunit assembly in vitro. These studies have revealed that the DnaK (heat shock protein 70) chaperone system can facilitate 30S subunit assembly in vitro. The 30S subunits, formed in the presence of the chaperones under otherwise non-permissive conditions, are highly similar to 30S subunits formed under standard reconstitution conditions. It has become evident that the manner in which the "factor-assembled" 30S subunits are purified is critical for monitoring formation of functional ribosomal particles. Given that methodologies for in vitro reconstitution and functional analysis of ribosomal subunits have been described in detail previously, this manuscript will focus on isolation of functional 30S subunits that have been assembled in the presence of exogenous factors in vitro. Also, recent efforts toward understanding the roles of exogenous factors in 50S subunit and eukaryotic ribosome assembly will be briefly discussed.

摘要

大肠杆菌核糖体亚基在高度优化的条件下可在体外进行重组。这些重组系统已被证明对核糖体亚基组装的研究具有极高价值。虽然大肠杆菌核糖体亚基能在体外自我组装,但关于在体内功能性亚基形成过程中起作用的核糖体外部组装因子的存在,一直存在诸多推测。最近,已实施一种生化检测方法来鉴定在体外促进30S亚基组装中单个关键步骤的因子。这些研究表明,DnaK(热休克蛋白70)伴侣系统可在体外促进30S亚基组装。在原本不允许的条件下,在伴侣蛋白存在时形成的30S亚基与在标准重组条件下形成的30S亚基高度相似。显然,“因子组装”的30S亚基的纯化方式对于监测功能性核糖体颗粒的形成至关重要。鉴于之前已详细描述了核糖体亚基体外重组和功能分析的方法,本手稿将重点关注在体外存在外源因子的情况下组装的功能性30S亚基的分离。此外,还将简要讨论最近在理解外源因子在50S亚基和真核核糖体组装中的作用方面所做的努力。

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