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RNA聚合酶的集体运动。核心酶、延伸复合物和全酶的分析。

Collective motions of RNA polymerases. Analysis of core enzyme, elongation complex and holoenzyme.

作者信息

Yildirim Y, Doruker P

机构信息

Department of Chemical Engineering and Polymer Research Center, Bogazici University, Bebek, Istanbul 34342, Turkey.

出版信息

J Biomol Struct Dyn. 2004 Dec;22(3):267-80. doi: 10.1080/07391102.2004.10507000.

Abstract

The anisotropic network model (ANM), a coarse-grained normal mode analysis, is used to study the vibrational dynamics of RNA polymerases (RNAP) around the native states. The theoretical temperature factors obtained from ANM are in conformity with the experimental values for yeast and bacterial RNAP structures in free and complex forms. In the low-frequency collective modes that are related to biological function, both bacterial and yeast RNAPs with a crab claw shape display an opening/closing of the cleft due to the rigid-body motion of the clamp (bottom pincer), which has been also predicted by experiments, together with the motion of the top pincer. Even though slightly lower fluctuations are observed in the elongation complex of yeast RNAP, similar clamp motion still exists in collective modes, which should be concerted with the flexible switches and the bridge helix in driving the transcription process, pointing at the possibility of a ratchet-like mechanism. Two different bacterial holoenzyme (HE) structures are studied, which may have functional significance at different stages of transcription initiation. In a specific closed conformation of the HE, the clamp and top pincer are highly immobilized due to interactions with the sigma subunit. In contrast, the deformation of the top pincer is not inhibited in a relatively open conformation of another HE, which may help load the DNA into the cleft during transcription initiation, even though the clamp motion is still inhibited.

摘要

各向异性网络模型(ANM)是一种粗粒度的正常模式分析方法,用于研究RNA聚合酶(RNAP)在天然状态附近的振动动力学。从ANM获得的理论温度因子与酵母和细菌RNAP结构在游离和复合形式下的实验值相符。在与生物学功能相关的低频集体模式中,具有蟹钳形状的细菌和酵母RNAP由于夹子(底部钳)的刚体运动,都会显示出裂隙的打开/关闭,这一点也已被实验预测到,同时还有顶部钳的运动。尽管在酵母RNAP的延伸复合物中观察到的波动略低,但在集体模式中仍存在类似的夹子运动,这在驱动转录过程中应与柔性开关和桥螺旋协同作用,这表明存在棘轮样机制的可能性。研究了两种不同的细菌全酶(HE)结构,它们在转录起始的不同阶段可能具有功能意义。在HE的特定封闭构象中,由于与σ亚基的相互作用,夹子和顶部钳高度固定。相比之下,在另一种HE的相对开放构象中,顶部钳的变形没有受到抑制,这可能有助于在转录起始期间将DNA加载到裂隙中,尽管夹子运动仍然受到抑制。

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