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在 GDP、GTP 或 ppGpp 存在的情况下,ppGpp 与 EF-G 或 IF2 的结合以及起始 tRNA 与游离 IF2 的结合的热力学特性。

Thermodynamic characterization of ppGpp binding to EF-G or IF2 and of initiator tRNA binding to free IF2 in the presence of GDP, GTP, or ppGpp.

机构信息

Engelhardt Institute of Molecular Biology, Russian Academy of Sciences, Vavilov St. 32, Moscow 119991, Russia.

出版信息

J Mol Biol. 2010 Oct 8;402(5):838-46. doi: 10.1016/j.jmb.2010.08.016. Epub 2010 Aug 14.

Abstract

In addition to their natural substrates GDP and GTP, the bacterial translational GTPases initiation factor (IF) 2 and elongation factor G (EF-G) interact with the alarmone molecule guanosine tetraphosphate (ppGpp), which leads to GTPase inhibition. We have used isothermal titration calorimetry to determine the affinities of ppGpp for IF2 and EF-G at a temperature interval of 5-25 °C. We find that ppGpp has a higher affinity for IF2 than for EF-G (1.7-2.8 μM K(d)versus 9.1-13.9 μM K(d) at 10-25 °C), suggesting that during stringent response in vivo, IF2 is more responsive to ppGpp than to EF-G. We investigated the effects of ppGpp, GDP, and GTP on IF2 interactions with fMet-tRNA(fMet) demonstrating that IF2 binds to initiator tRNA with submicromolar K(d) and that affinity is altered by the G nucleotides only slightly. This--in conjunction with earlier reports on IF2 interactions with fMet-tRNA(fMet) in the context of the 30S initiation complex, where ppGpp was suggested to strongly inhibit fMet-tRNA(fMet) binding and GTP was suggested to strongly promote fMet-tRNA(fMet) binding--sheds new light on the mechanisms of the G-nucleotide-regulated fMet-tRNA(fMet) selection.

摘要

除了它们的天然底物 GDP 和 GTP 之外,细菌翻译起始因子 (IF) 2 和延伸因子 G (EF-G) 还与警报素分子四磷酸鸟苷 (ppGpp) 相互作用,导致 GTP 酶抑制。我们使用等温滴定量热法在 5-25°C 的温度范围内确定了 ppGpp 与 IF2 和 EF-G 的亲和力。我们发现 ppGpp 与 IF2 的亲和力高于 EF-G(1.7-2.8 μM K(d) 与 9.1-13.9 μM K(d),在 10-25°C),这表明在体内严格响应期间,IF2 对 ppGpp 的反应比对 EF-G 更敏感。我们研究了 ppGpp、GDP 和 GTP 对 IF2 与 fMet-tRNA(fMet) 相互作用的影响,证明 IF2 以亚毫摩尔 K(d) 与起始 tRNA 结合,并且仅略微改变 G 核苷酸的亲和力。这——结合早先关于 IF2 在 30S 起始复合物中与 fMet-tRNA(fMet) 的相互作用的报告,其中 ppGpp 被认为强烈抑制 fMet-tRNA(fMet) 结合,而 GTP 被认为强烈促进 fMet-tRNA(fMet) 结合——为 G 核苷酸调节的 fMet-tRNA(fMet) 选择机制提供了新的见解。

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