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来自螺旋轮丝链霉菌的互隔交链孢酚生物合成基因簇的表征揭示了对二烷基马来酸酐和聚酮生物合成的新见解。

Characterization of the tautomycin biosynthetic gene cluster from Streptomyces spiroverticillatus unveiling new insights into dialkylmaleic anhydride and polyketide biosynthesis.

作者信息

Li Wenli, Ju Jianhua, Rajski Scott R, Osada Hiroyuki, Shen Ben

机构信息

Division of Pharmaceutical Sciences, University of Wisconsin-Madison, Madison, Wisconsin 53705, USA.

出版信息

J Biol Chem. 2008 Oct 17;283(42):28607-17. doi: 10.1074/jbc.M804279200. Epub 2008 Aug 15.

DOI:10.1074/jbc.M804279200
PMID:18708355
原文链接:https://pmc.ncbi.nlm.nih.gov/articles/PMC2568922/
Abstract

Tautomycin (TTM) is a highly potent and specific protein phosphatase inhibitor isolated from Streptomyces spiroverticillatus. The biological activity of TTM makes it an important lead for drug discovery, whereas its spiroketal-containing polyketide chain and rare dialkylmaleic anhydride moiety draw attention to novel biosynthetic chemistries responsible for its production. To elucidate the biosynthetic machinery associated with these novel molecular features, the ttm biosynthetic gene cluster from S. spiroverticillatus was isolated and characterized, and its involvement in TTM biosynthesis was confirmed by gene inactivation and complementation experiments. The ttm cluster was localized to a 86-kb DNA region, consisting of 20 open reading frames that encode three modular type I polyketide synthases (TtmHIJ), one type II thioesterase (TtmT), five proteins for methoxymalonyl-S-acyl carrier protein biosynthesis (Ttm-ABCDE), eight proteins for dialkylmaleic anhydride biosynthesis and regulation (TtmKLMNOPRS), as well as two additional regulatory proteins (TtmF and TtmQ) and one tailoring enzyme (TtmG). A model for TTM biosynthesis is proposed based on functional assignments from sequence analysis, which agrees well with previous feeding experiments, and has been further supported by in vivo gene inactivation experiments. These findings set the stage to fully investigate TTM biosynthesis and to biosynthetically engineer new TTM analogs.

摘要

互隔交链孢酚(TTM)是一种从浅绿链霉菌中分离出的高效且特异的蛋白磷酸酶抑制剂。TTM的生物活性使其成为药物研发的重要先导化合物,而其含螺缩酮的聚酮链和罕见的二烷基马来酸酐部分则引发了对负责其产生的新型生物合成化学的关注。为阐明与这些新型分子特征相关的生物合成机制,从浅绿链霉菌中分离并鉴定了ttm生物合成基因簇,并通过基因失活和互补实验证实了其参与TTM的生物合成。ttm基因簇定位于一个86 kb的DNA区域,由20个开放阅读框组成,这些开放阅读框编码三种模块化I型聚酮合酶(TtmHIJ)、一种II型硫酯酶(TtmT)、五种参与甲氧基丙二酰-S-酰基载体蛋白生物合成的蛋白质(Ttm-ABCDE)、八种参与二烷基马来酸酐生物合成和调控的蛋白质(TtmKLMNOPRS),以及另外两种调控蛋白(TtmF和TtmQ)和一种修饰酶(TtmG)。基于序列分析的功能分配提出了一个TTM生物合成模型,该模型与先前的饲喂实验结果吻合良好,并得到了体内基因失活实验的进一步支持。这些发现为全面研究TTM生物合成以及通过生物合成工程制备新的TTM类似物奠定了基础。

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