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通过对一种DNA拓扑异构酶的冷冻电镜研究对酶催化作用的统一观点。

A unified view on enzyme catalysis by cryo-EM study of a DNA topoisomerase.

作者信息

Chang Chiung-Wen Mary, Wang Shun-Chang, Wang Chun-Hsiung, Pang Allan H, Yang Cheng-Han, Chang Yao-Kai, Wu Wen-Jin, Tsai Ming-Daw

机构信息

Institute of Biological Chemistry, Academia Sinica, Taipei, 115, Taiwan.

Institute of Biochemistry and Molecular Biology, China Medical University, Taichung, Taiwan.

出版信息

Commun Chem. 2024 Feb 28;7(1):45. doi: 10.1038/s42004-024-01129-y.

Abstract

The theories for substrate recognition in enzyme catalysis have evolved from lock-key to induced fit, then conformational selection, and conformational selection followed by induced fit. However, the prevalence and consensus of these theories require further examination. Here we use cryogenic electron microscopy and African swine fever virus type 2 topoisomerase (AsfvTop2) to demonstrate substrate binding theories in a joint and ordered manner: catalytic selection by the enzyme, conformational selection by the substrates, then induced fit. The apo-AsfvTop2 pre-exists in six conformers that comply with the two-gate mechanism directing DNA passage and release in the Top2 catalytic cycle. The structures of AsfvTop2-DNA-inhibitor complexes show that substantial induced-fit changes occur locally from the closed apo-conformer that however is too far-fetched for the open apo-conformer. Furthermore, the ATPase domain of AsfvTop2 in the MgAMP-PNP-bound crystal structures coexist in reduced and oxidized forms involving a disulfide bond, which can regulate the AsfvTop2 function.

摘要

酶催化中底物识别的理论已从锁钥模型发展到诱导契合模型,然后是构象选择模型,以及构象选择后诱导契合模型。然而,这些理论的普遍性和共识性仍需进一步研究。在此,我们利用低温电子显微镜和2型非洲猪瘟病毒拓扑异构酶(AsfvTop2)以联合且有序的方式展示底物结合理论:酶的催化选择、底物的构象选择,然后是诱导契合。无底物的AsfvTop2预先存在于六种构象中,这些构象符合指导DNA在Top2催化循环中通过和释放的双门机制。AsfvTop2-DNA-抑制剂复合物的结构表明,从封闭的无底物构象会局部发生大量诱导契合变化,然而对于开放的无底物构象来说,这种变化过于牵强。此外,MgAMP-PNP结合晶体结构中的AsfvTop2的ATP酶结构域以涉及二硫键的还原和氧化形式共存,这可以调节AsfvTop2的功能。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/b523/10901890/5782df56cc64/42004_2024_1129_Fig1_HTML.jpg

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