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在溶液中 GDPNP 和 GDP 结合时翻译起始因子 IF2 的结构转变。

Structural transitions of translation initiation factor IF2 upon GDPNP and GDP binding in solution.

机构信息

Department of Molecular Biology, Aarhus University, Gustav Wieds Vej 10, DK-8000 Aarhus C, Denmark.

出版信息

Biochemistry. 2011 Nov 15;50(45):9779-87. doi: 10.1021/bi200938q. Epub 2011 Oct 19.

Abstract

Three protein factors ensure rapid and accurate initiation of translation in bacteria. Translation initiation factor IF2 is a ribosome-dependent GTPase, which is important for correct positioning of initiator tRNA on the 30S subunit as well as ribosomal subunit joining. The solution structure of the free C-terminal part of IF2 (IF2C, comprising domains IV to VI-2) was previously determined by small-angle X-ray scattering (SAXS) [Rasmussen, L. C., et al. (2008) Biochemistry 47, 5590-5598]. In this study, adding GDP or nonhydrolyzable GTP analogue GDPNP to the protein in solution caused structural changes in the protein, in agreement with recent data determined via isothermal titration calorimetry [Hauryliuk, V., et al. (2009) J. Mol. Biol. 394, 621-626]. The p(r) function indicated an elongated conformation supported by radii of gyration of 40.1 and 44.9 Å and maximum dimensions of ~125 and ~150 Å for IF2C with GDPNP and GDP, respectively. The SAXS data were used to model the structure of IF2C bound to either GDPNP or GDP. The structural transitions of IF2C upon GDPNP binding and following nucleotide hydrolysis support the concept of cofactor-dependent conformational switching rather than the classical model for GTPase activity.

摘要

三种蛋白质因子确保了细菌中翻译的快速和准确起始。翻译起始因子 IF2 是一种依赖于核糖体的 GTP 酶,它对于正确定位起始 tRNA 在 30S 亚基上以及核糖体亚基的结合非常重要。IF2 的游离 C 端部分(IF2C,包含结构域 IV 至 VI-2)的溶液结构先前通过小角 X 射线散射(SAXS)确定[Rasmussen,LC 等人。(2008)生物化学 47,5590-5598]。在这项研究中,在溶液中的蛋白质中添加 GDP 或非水解 GTP 类似物 GDPNP 会导致蛋白质的结构发生变化,这与最近通过等温滴定量热法确定的数据一致[Hauryliuk,V. 等人。(2009)J. Mol. Biol. 394,621-626]。p(r) 函数表明,IF2C 与 GDPNP 和 GDP 结合时,分别支持旋转半径为 40.1 和 44.9 Å 以及最大尺寸约为 125 和 150 Å 的伸长构象。SAXS 数据用于模拟 IF2C 与 GDPNP 或 GDP 结合的结构。IF2C 在 GDPNP 结合和随后的核苷酸水解时的结构转变支持了辅助因子依赖性构象转换的概念,而不是经典的 GTP 酶活性模型。

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