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具有广泛底物混杂性的环状二肽烯基转移酶的结构和催化机制。

Structure and catalytic mechanism of a cyclic dipeptide prenyltransferase with broad substrate promiscuity.

机构信息

Interfakultäres Institut für Biochemie, Universität Tübingen, Hoppe-Seyler-Str. 4, 72076 Tübingen, Germany.

出版信息

J Mol Biol. 2012 Sep 7;422(1):87-99. doi: 10.1016/j.jmb.2012.05.033. Epub 2012 Jun 6.

Abstract

Fungal indole prenyltransferases (PTs) typically act on specific substrates, and they are able to prenylate their target compounds with remarkably high regio- and stereoselectivity. Similar to several indole PTs characterized to date, the cyclic dipeptide N-prenyltransferase (CdpNPT) is able to prenylate a range of diverse substrates, thus exhibiting an unusually broad substrate promiscuity. To define the structural basis for this promiscuity, we have determined crystal structures of unliganded CdpNPT and of a ternary complex of CdpNPT bound to (S)-benzodiazepinedione and thiolodiphosphate. Analysis of the structures reveals a limited number of specific interactions with (S)-benzodiazepinedione, which projects into a largely hydrophobic surface. This surface can also accommodate other substrates, explaining the ability of the enzyme to prenylate a range of compounds. The location of the bound substrates suggests a likely reaction mechanism for the conversion of (S)-benzodiazepinedione. Structure-guided mutagenesis experiments confirm that, in addition to (S)-benzodiazepinedione, CdpNPT can also act on (R)-benzodiazepinedione and several cyclic dipeptides, albeit with relaxed specificity. Finally, nuclear magnetic resonance spectroscopy demonstrates that CdpNPT is a C-3 reverse PT that catalyzes the formation of C-3β prenylated indolines from diketopiperazines of tryptophan-containing cyclic dipeptides.

摘要

真菌吲哚 prenyltransferase(PT)通常作用于特定的底物,并且能够以高度区域和立体选择性的方式将其目标化合物 prenyl 化。与迄今为止表征的几种吲哚 PT 相似,环状二肽 N-prenyltransferase(CdpNPT)能够 prenylate 一系列不同的底物,因此表现出异常广泛的底物混杂性。为了定义这种混杂性的结构基础,我们已经确定了未配位的 CdpNPT 的晶体结构以及与(S)-苯并二氮䓬二酮和硫代二磷酸结合的三元复合物的晶体结构。结构分析揭示了与(S)-苯并二氮䓬二酮的少数特定相互作用,该二酮投影到一个主要疏水面上。该表面还可以容纳其他底物,解释了酶能够 prenylate 一系列化合物的能力。结合底物的位置表明了(S)-苯并二氮䓬二酮转化的可能反应机制。基于结构的诱变实验证实,除了(S)-苯并二氮䓬二酮外,CdpNPT 还可以作用于(R)-苯并二氮䓬二酮和几种环状二肽,尽管特异性有所放宽。最后,核磁共振波谱证明 CdpNPT 是一种 C-3 反向 PT,它可以从含有色氨酸的环状二肽的二酮哌嗪中催化 C-3βprenylated indolines 的形成。

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