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定点诱变与底物兼容性以揭示植物氧化角鲨烯环化酶的结构-功能关系。

Site-directed mutagenesis and substrate compatibility to reveal the structure-function relationships of plant oxidosqualene cyclases.

作者信息

Chen Kuan, Zhang Meng, Ye Min, Qiao Xue

机构信息

State Key Laboratory of Natural and Biomimetic Drugs, School of Pharmaceutical Sciences, Peking University, 38 Xueyuan Road, Beijing 100191, China.

出版信息

Nat Prod Rep. 2021 Dec 15;38(12):2261-2275. doi: 10.1039/d1np00015b.

Abstract

Covering: up to May 2020Oxidosqualene cyclases (OSCs) catalyze one of the most complex polycyclization reactions in nature, using the linear 2,3-oxidosqualene to generate an array of triterpene skeletons in plants. Despite the structural diversity of the products, the protein sequences of plant OSCs are highly conserved, where a few key amino acids could govern the product selectivity. Due to the absence of crystal structures, site-directed mutagenesis and substrate structural modification become key approaches to understand the cyclization mechanism. In this review, 98 mutation sites in 25 plant OSCs have been summarized, and the conserved key residues have been identified by sequence alignment. Structure-function relationships are further discussed. Meanwhile, the substrate selectivity has been summarized to probe the active site cavity of plant OSCs. A total of 77 references are included.

摘要

涵盖范围

截至2020年5月

氧化角鲨烯环化酶(OSCs)催化自然界中最复杂的多环化反应之一,利用线性的2,3-氧化角鲨烯在植物中生成一系列三萜骨架。尽管产物具有结构多样性,但植物OSCs的蛋白质序列高度保守,少数关键氨基酸可决定产物选择性。由于缺乏晶体结构,定点诱变和底物结构修饰成为理解环化机制的关键方法。在本综述中,总结了25种植物OSCs中的98个突变位点,并通过序列比对鉴定了保守的关键残基。进一步讨论了结构-功能关系。同时,总结了底物选择性以探究植物OSCs的活性位点空腔。共纳入77篇参考文献。

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