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李斯特菌冷休克蛋白的结构和动态特征,一种嗜冷细菌。

Structural and dynamic features of cold-shock proteins of Listeria monocytogenes, a psychrophilic bacterium.

机构信息

Department of Bioscience and Biotechnology, Bio/Molecular Informatics Center, Konkuk University, Seoul 143-701, South Korea.

出版信息

Biochemistry. 2013 Apr 9;52(14):2492-504. doi: 10.1021/bi301641b. Epub 2013 Apr 1.

DOI:10.1021/bi301641b
PMID:23506337
Abstract

Cold-shock proteins (Csps), proteins expressed when the ambient temperature drops below the growth-supporting temperature, bind to single-stranded nucleic acids and act as RNA chaperones to regulate translation. Listeria monocytogenes is a psychrophilic food-borne pathogen that is problematic for the food industry. Structures of Csps from psychrophilic bacteria have not yet been studied. Despite dramatic differences in the thermostability of Csps of various thermophilic microorganisms, these proteins share a high degree of primary sequence homology and a high degree of three-dimensional structural similarity. Here, we investigated the structural and dynamic features as well as the thermostability of L. monocytogenes CspA (Lm-CspA). Lm-CspA has a five-stranded β-barrel structure with hydrophobic core packing and two salt bridges. When heptathymidine (dT(7)) binds, values for the heteronuclear nuclear Overhauser effect and order parameters of residues in surface loop regions near nucleic acid binding sites increase dramatically. Moreover, Carr-Purcell-Meiboom-Gill experiments showed that slow motions observed for the nucleic acid binding residues K7, W8, F15, F27, and R56 disappeared in Lm-CspA-dT(7). Lm-CspA is less thermostable than mesophilic and thermophilic Csps, with a lower melting temperature (40 °C). The structural flexibility that accompanies longer surface loops and less hydrophobic core packing and a number of salt bridges and unfavorable electrostatic repulsion are likely key factors in the low thermostability of Lm-CspA. This implies that the large conformational flexibility of psychrophilic Lm-CspA, which more easily accommodates nucleic acids at low temperature, is required for RNA chaperone function under cold-shock conditions and for the cold adaptation of L. monocytogenes.

摘要

冷休克蛋白(Csps)是在环境温度低于支持生长的温度时表达的蛋白质,它们与单链核酸结合,作为 RNA 伴侣来调节翻译。李斯特菌是一种嗜冷食源性病原体,给食品工业带来了问题。目前尚未研究过来自嗜冷细菌的 Csp 结构。尽管各种嗜热微生物的 Csp 在热稳定性方面存在显著差异,但这些蛋白质具有高度的一级序列同源性和高度的三维结构相似性。在这里,我们研究了李斯特菌 CspA(Lm-CspA)的结构和动态特性以及热稳定性。Lm-CspA 具有五股β-桶结构,具有疏水性核心包装和两个盐桥。当七胸腺嘧啶(dT(7))结合时,核酸结合位点附近表面环区域中残基的异核核 Overhauser 效应和顺序参数值会显著增加。此外,Carr-Purcell-Meiboom-Gill 实验表明,在 Lm-CspA-dT(7)中,与核酸结合残基 K7、W8、F15、F27 和 R56 相关的缓慢运动消失了。Lm-CspA 的热稳定性低于中温和嗜热 Csps,熔点较低(40°C)。伴随更长的表面环、更少的疏水性核心包装以及更多的盐桥和不利的静电排斥的结构灵活性可能是 Lm-CspA 低热稳定性的关键因素。这意味着在冷休克条件下,作为 RNA 伴侣的功能和李斯特菌的冷适应需要,来自嗜冷李斯特菌的 Lm-CspA 的大构象灵活性更容易在低温下容纳核酸。

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