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HD结构域金属蛋白超家族:一种具有多样化学性质的明显通用蛋白质支架

The HD-Domain Metalloprotein Superfamily: An Apparent Common Protein Scaffold with Diverse Chemistries.

作者信息

Langton Michelle, Sun Sining, Ueda Chie, Markey Max, Chen Jiahua, Paddy Isaac, Jiang Paul, Chin Natalie, Milne Amy, Pandelia Maria-Eirini

机构信息

Department of Biochemistry, Brandeis University, 415 South Street, Waltham, MA 02453, USA.

出版信息

Catalysts. 2020 Oct;10(10). doi: 10.3390/catal10101191. Epub 2020 Oct 15.

Abstract

The histidine-aspartate (HD)-domain protein superfamily contains metalloproteins that share common structural features but catalyze vastly different reactions ranging from oxygenation to hydrolysis. This chemical diversion is afforded by (i) their ability to coordinate most biologically relevant transition metals in mono-, di-, and trinuclear configurations, (ii) sequence insertions or the addition of supernumerary ligands to their active sites, (iii) auxiliary substrate specificity residues vicinal to the catalytic site, (iv) additional protein domains that allosterically regulate their activities or have catalytic and sensory roles, and (v) their ability to work with protein partners. More than 500 structures of HD-domain proteins are available to date that lay out unique structural features which may be indicative of function. In this respect, we describe the three known classes of HD-domain proteins (hydrolases, oxygenases, and lyases) and identify their apparent traits with the aim to portray differences in the molecular details responsible for their functional divergence and reconcile existing notions that will help assign functions to yet-to-be characterized proteins. The present review collects data that exemplify how nature tinkers with the HD-domain scaffold to afford different chemistries and provides insight into the factors that can selectively modulate catalysis.

摘要

组氨酸-天冬氨酸(HD)结构域蛋白超家族包含金属蛋白,这些金属蛋白具有共同的结构特征,但催化的反应却大不相同,从氧化反应到水解反应都有。这种化学功能的转变是由以下因素实现的:(i)它们能够以单核、双核和三核构型配位大多数与生物相关的过渡金属;(ii)在其活性位点进行序列插入或添加多余的配体;(iii)催化位点附近的辅助底物特异性残基;(iv)其他能变构调节其活性或具有催化和传感作用的蛋白质结构域;(v)它们与蛋白质伙伴协同工作的能力。迄今为止,已有500多种HD结构域蛋白的结构,这些结构展示了可能指示功能的独特结构特征。在这方面,我们描述了HD结构域蛋白的三类已知类型(水解酶、加氧酶和裂合酶),并确定它们的明显特征,目的是描绘出导致其功能差异的分子细节中的差异,并调和现有的概念,这将有助于为尚未表征的蛋白质赋予功能。本综述收集了一些数据,这些数据例证了自然界如何对HD结构域支架进行调整以实现不同的化学反应,并深入了解能够选择性调节催化作用的因素。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/4a8e/8177086/ab6ce3e80d0c/nihms-1703855-f0001.jpg

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