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植物1家族糖基转移酶的糖供体特异性。

The sugar donor specificity of plant family 1 glycosyltransferases.

作者信息

Gharabli Hani, Welner Ditte Hededam

机构信息

The Novo Nordisk Center for Biosustainability, Technical University of Denmark, Kongens Lyngby, Denmark.

出版信息

Front Bioeng Biotechnol. 2024 May 2;12:1396268. doi: 10.3389/fbioe.2024.1396268. eCollection 2024.

Abstract

Plant family 1 glycosyltransferases (UGTs) represent a formidable tool to produce valuable natural and novel glycosides. Their regio- and stereo-specific one-step glycosylation mechanism along with their inherent wide acceptor scope are desirable traits in biotechnology. However, their donor scope and specificity are not well understood. Since different sugars have different properties and , the ability to easily glycodiversify target acceptors is desired, and this depends on our improved understanding of the donor binding site. In the aim to unlock the full potential of UGTs, studies have attempted to elucidate the structure-function relationship governing their donor specificity. These efforts have revealed a complex phenomenon, and general principles valid for multiple enzymes are elusive. Here, we review the studies of UGT donor specificity, and attempt to group the information into key concepts which can help shape future research. We zoom in on the family-defining PSPG motif, on two loop residues reported to interact with the C6 position of the sugar, and on the role of active site arginines in donor specificity. We continue to discuss attempts to alter and expand the donor specificity by enzyme engineering, and finally discuss future research directions.

摘要

植物家族1糖基转移酶(UGTs)是生产有价值的天然糖苷和新型糖苷的强大工具。它们的区域和立体特异性一步糖基化机制以及固有的广泛受体范围是生物技术中理想的特性。然而,它们的供体范围和特异性尚未得到充分了解。由于不同的糖具有不同的性质,并且需要能够轻松地对目标受体进行糖基多样化,这取决于我们对供体结合位点的深入理解。为了充分发挥UGTs的潜力,研究试图阐明控制其供体特异性的结构-功能关系。这些努力揭示了一个复杂的现象,适用于多种酶的一般原则难以捉摸。在这里,我们回顾了关于UGT供体特异性的研究,并试图将这些信息归纳为关键概念,以帮助指导未来的研究。我们重点关注家族定义的PSPG基序、据报道与糖的C6位置相互作用的两个环残基以及活性位点精氨酸在供体特异性中的作用。我们继续讨论通过酶工程改变和扩大供体特异性的尝试,最后讨论未来的研究方向。

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