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作为冷适应策略的增加灵活性:冷活性和热活性尿嘧啶DNA糖基化酶的比较分子动力学研究

Increased flexibility as a strategy for cold adaptation: a comparative molecular dynamics study of cold- and warm-active uracil DNA glycosylase.

作者信息

Olufsen Magne, Smalås Arne O, Moe Elin, Brandsdal Bjørn O

机构信息

Norwegian Structural Biology Centre, University of Tromsø, N-9037 Tromsø, Norway.

出版信息

J Biol Chem. 2005 May 6;280(18):18042-8. doi: 10.1074/jbc.M500948200. Epub 2005 Mar 3.

DOI:10.1074/jbc.M500948200
PMID:15749696
Abstract

Uracil DNA glycosylase (UDG) is a DNA repair enzyme in the base excision repair pathway and removes uracil from the DNA strand. Atlantic cod UDG (cUDG), which is a cold-adapted enzyme, has been found to be up to 10 times more catalytically active in the temperature range 15-37 degrees C as compared with the warm-active human counterpart. The increased catalytic activity of cold-adapted enzymes as compared with their mesophilic homologues are partly believed to be caused by an increase in the structural flexibility. However, no direct experimental evidence supports the proposal of increased flexibility of cold-adapted enzymes. We have used molecular dynamics simulations to gain insight into the structural flexibility of UDG. The results from these simulations show that an important loop involved in DNA recognition (the Leu(272) loop) is the most flexible part of the cUDG structure and that the human counterpart has much lower flexibility in the Leu(272) loop. The flexibility in this loop correlates well with the experimental k(cat)/K(m) values. Thus, the data presented here add strong support to the idea that flexibility plays a central role in adaptation to cold environments.

摘要

尿嘧啶DNA糖基化酶(UDG)是碱基切除修复途径中的一种DNA修复酶,可从DNA链中去除尿嘧啶。大西洋鳕鱼UDG(cUDG)是一种适应低温的酶,已发现其在15至37摄氏度的温度范围内,催化活性比适应温暖环境的人类对应酶高出10倍。与中温同源物相比,适应低温的酶催化活性增加部分被认为是由于结构灵活性增加所致。然而,没有直接的实验证据支持适应低温的酶灵活性增加这一观点。我们利用分子动力学模拟来深入了解UDG的结构灵活性。这些模拟结果表明,参与DNA识别的一个重要环(Leu(272)环)是cUDG结构中最灵活的部分,而人类对应酶在Leu(272)环中的灵活性要低得多。该环的灵活性与实验测得的k(cat)/K(m)值密切相关。因此,此处给出的数据有力支持了灵活性在适应寒冷环境中起核心作用这一观点。

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