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转录终止因子Rho的机械化学

Mechanochemistry of transcription termination factor Rho.

作者信息

Adelman Joshua L, Jeong Yong-Joo, Liao Jung-Chi, Patel Gayatri, Kim Dong-Eun, Oster George, Patel Smita S

机构信息

Biophysics Graduate Group, University of California, Berkeley, Berkeley, California 94720, USA.

出版信息

Mol Cell. 2006 Jun 9;22(5):611-21. doi: 10.1016/j.molcel.2006.04.022.

Abstract

Rho is a ring-shaped hexameric motor protein that translocates along nascent mRNA transcript and terminates transcription of select genes in bacteria. Using a numerical optimization algorithm that simultaneously fits all of the presteady-state ATPase kinetic data, we determine how Rho utilizes the chemical energy of ATP hydrolysis to translocate RNA. A random hydrolysis mechanism is ruled out by the observed inhibition of ATPase in a mixed hexamer containing wt and an inactive Rho mutant. We propose a mechanism in which (1) all six subunits are catalytically competent and hydrolyze ATP sequentially, (2) translocation of RNA is driven by the weak to tight binding transition of nucleotide in the catalytic site, (3) hydrolysis is coordinated between adjacent subunits by the transmission of stress via the catalytic arginine finger, (4) hydrolysis weakens the affinity of a subunit for RNA, and (5) the slow release of inorganic phosphate is controlled by changes in circumferential stress around the ring.

摘要

Rho是一种环状六聚体马达蛋白,它沿着新生的mRNA转录本移位,并终止细菌中特定基因的转录。我们使用一种数值优化算法同时拟合所有稳态前ATP酶动力学数据,来确定Rho如何利用ATP水解的化学能使RNA移位。在含有野生型和无活性Rho突变体的混合六聚体中观察到的ATP酶抑制作用排除了随机水解机制。我们提出了一种机制,其中:(1)所有六个亚基都具有催化活性并依次水解ATP;(2)RNA的移位由催化位点中核苷酸从弱结合到紧密结合的转变驱动;(3)水解通过催化精氨酸指传递应力在相邻亚基之间进行协调;(4)水解减弱了亚基对RNA的亲和力;(5)无机磷酸的缓慢释放由环周围周向应力的变化控制。

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