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用于萜类骨架糖基化的新型生物催化剂的发现。

Discovery of new biocatalysts for the glycosylation of terpenoid scaffolds.

作者信息

Caputi Lorenzo, Lim Eng-Kiat, Bowles Dianna J

机构信息

CNAP, Department of Biology, University of York, York, UK.

出版信息

Chemistry. 2008;14(22):6656-62. doi: 10.1002/chem.200800548.

Abstract

The synthesis of terpenoid glycosides typically uses a chemical strategy since few biocatalysts have been identified that recognise these scaffolds. In this study, a platform of 107 recombinant glycosyltransferases (GTs), comprising the multigene family of small molecule GTs of Arabidopsis thaliana have been screened against a range of model terpenoid acceptors to identify those enzymes with high activity. Twenty-seven GTs are shown to glycosylate a diversity of mono-, sesqui- and diterpenes, such as geraniol, perillyl alcohol, artemisinic acid and retinoic acid. Certain enzymes showing substantial sequence similarity recognise terpenoids containing a primary alcohol, irrespective of the linear or cyclical structure of the scaffold; other GTs glycosylate scaffolds containing secondary and tertiary alcohols; the carboxyl group of other terpenoids also represents a feature that is recognized by GTs previously known to form glucose esters with many different compounds. These data underpin the rapid prediction of potential biocatalysts from GT sequence information. To explore the potential of GTs as biocatalysts, their use for the production of terpenoid glycosides was investigated by using a microbial-based whole-cell biotransformation system capable of regenerating the cofactor, UDP-glucose. A high cell density fermentation system was shown to produce several hundred milligrams of a model terpenoid, geranyl-glucoside. The activities of the GTs are discussed in relation to their substrate recognition and their utility in biotransformations as a complement or alternative to chemical synthesis.

摘要

萜类糖苷的合成通常采用化学策略,因为很少有已鉴定出的生物催化剂能够识别这些支架结构。在本研究中,针对一系列萜类模型受体,筛选了一个由107种重组糖基转移酶(GTs)组成的平台,这些酶来自拟南芥小分子GTs的多基因家族,以鉴定具有高活性的酶。结果表明,27种GTs能够糖基化多种单萜、倍半萜和二萜,如香叶醇、紫苏醇、青蒿酸和视黄酸。某些序列相似度较高的酶能够识别含有伯醇的萜类化合物,而不论其支架结构是线性还是环状;其他GTs则能糖基化含有仲醇和叔醇的支架结构;其他萜类化合物的羧基也是GTs识别的一个特征,这些GTs此前已知能够与许多不同化合物形成葡萄糖酯。这些数据为从GT序列信息快速预测潜在生物催化剂提供了依据。为了探索GTs作为生物催化剂的潜力,通过使用能够再生辅因子UDP-葡萄糖的基于微生物的全细胞生物转化系统,研究了它们在萜类糖苷生产中的应用。结果表明,高细胞密度发酵系统能够产生数百毫克的模型萜类化合物香叶基葡萄糖苷。本文讨论了GTs的活性与其底物识别的关系,以及它们在生物转化中作为化学合成的补充或替代方法的实用性。

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