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植物和人类 MORC 蛋白具有与 II 型拓扑异构酶相似的 DNA 修饰活性,但需要一个或多个额外的因素才能充分发挥活性。

Plant and Human MORC Proteins Have DNA-Modifying Activities Similar to Type II Topoisomerases, but Require One or More Additional Factors for Full Activity.

机构信息

1 Boyce Thompson Institute, Ithaca, NY 14853, U.S.A.

2 Institute for Cell and Molecular Biosciences, Newcastle University, NE2 4HH, U.K.; and.

出版信息

Mol Plant Microbe Interact. 2017 Feb;30(2):87-100. doi: 10.1094/MPMI-10-16-0208-R. Epub 2017 Feb 3.

Abstract

To elucidate one or more mechanisms through which microrchidia (MORC) proteins impact immunity, epigenetic gene silencing, and DNA modifications, the enzymatic activities of plant MORCs were characterized. Previously, we showed that plant MORC1s have ATPase and DNA endonuclease activities. Here, we demonstrate that plant MORCs have topoisomerase type II (topo II)-like activities, as they i) covalently bind DNA, ii) exhibit DNA-stimulated ATPase activity, iii) relax or nick supercoiled DNA, iv) catenate DNA, and v) decatenante kinetoplast DNA. Mutational analysis of tomato SlMORC1 suggests that a K loop-like sequence is required to couple DNA binding to ATPase stimulation as well as for efficient SlMORC1's DNA relaxation and catenation activities and in planta suppression of INF1-induced cell death, which is related to immunity. Human MORCs were found to exhibit the same topo II-like DNA modification activities as their plant counterparts. In contrast to typical topo IIs, SlMORC1 appears to require one or more accessory factors to complete some of its enzymatic activities, since addition of tomato extracts were needed for ATP-dependent, efficient conversion of supercoiled DNA to nicked/relaxed DNA and catenanes and for formation of topoisomer intermediates. Both plant and human MORCs bind salicylic acid; this suppresses their decatenation but not relaxation activity.

摘要

为了阐明微线体(MORC)蛋白影响免疫、表观遗传基因沉默和 DNA 修饰的一个或多个机制,研究人员对植物 MORC 的酶活性进行了表征。此前,我们已经表明,植物 MORC1 具有 ATP 酶和 DNA 内切酶活性。在这里,我们证明植物 MORC 具有拓扑异构酶 II(topo II)样活性,因为它们:i)共价结合 DNA,ii)表现出 DNA 刺激的 ATP 酶活性,iii)松弛或切开超螺旋 DNA,iv)连环 DNA,以及 v)解开锥虫 DNA 的连环。番茄 SlMORC1 的突变分析表明,K 环样序列是将 DNA 结合与 ATP 酶刺激偶联以及 SlMORC1 高效的 DNA 松弛和连环活性以及在植物体内抑制与免疫相关的 INF1 诱导的细胞死亡所必需的。发现人类 MORC 具有与其植物对应物相同的拓扑异构酶 II 样 DNA 修饰活性。与典型的拓扑异构酶 I 不同,SlMORC1 似乎需要一个或多个辅助因子来完成其部分酶活性,因为需要添加番茄提取物才能在 ATP 依赖性条件下高效地将超螺旋 DNA 转化为切口/松弛的 DNA 和连环体,并形成拓扑异构酶中间体。植物和人类的 MORC 都结合水杨酸;这抑制了它们的解连环,但不抑制松弛活性。

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