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来自链霉菌属菌株ATCC 53650的kedarcidin生物合成基因簇的克隆与测序,为抗肿瘤抗生素烯二炔家族的生物合成提供了新见解。

Cloning and sequencing of the kedarcidin biosynthetic gene cluster from Streptoalloteichus sp. ATCC 53650 revealing new insights into biosynthesis of the enediyne family of antitumor antibiotics.

作者信息

Lohman Jeremy R, Huang Sheng-Xiong, Horsman Geoffrey P, Dilfer Paul E, Huang Tingting, Chen Yihua, Wendt-Pienkowski Evelyn, Shen Ben

机构信息

Department of Chemistry, The Scripps Research Institute, Jupiter, Florida 33458, USA.

出版信息

Mol Biosyst. 2013 Mar;9(3):478-91. doi: 10.1039/c3mb25523a. Epub 2013 Jan 29.

DOI:10.1039/c3mb25523a
PMID:23360970
原文链接:https://pmc.ncbi.nlm.nih.gov/articles/PMC3711097/
Abstract

Enediyne natural product biosynthesis is characterized by a convergence of multiple pathways, generating unique peripheral moieties that are appended onto the distinctive enediyne core. Kedarcidin (KED) possesses two unique peripheral moieties, a (R)-2-aza-3-chloro-β-tyrosine and an iso-propoxy-bearing 2-naphthonate moiety, as well as two deoxysugars. The appendage pattern of these peripheral moieties to the enediyne core in KED differs from the other enediynes studied to date with respect to stereochemical configuration. To investigate the biosynthesis of these moieties and expand our understanding of enediyne core formation, the biosynthetic gene cluster for KED was cloned from Streptoalloteichus sp. ATCC 53650 and sequenced. Bioinformatics analysis of the ked cluster revealed the presence of the conserved genes encoding for enediyne core biosynthesis, type I and type II polyketide synthase loci likely responsible for 2-aza-l-tyrosine and 3,6,8-trihydroxy-2-naphthonate formation, and enzymes known for deoxysugar biosynthesis. Genes homologous to those responsible for the biosynthesis, activation, and coupling of the l-tyrosine-derived moieties from C-1027 and maduropeptin and of the naphthonate moiety from neocarzinostatin are present in the ked cluster, supporting 2-aza-l-tyrosine and 3,6,8-trihydroxy-2-naphthoic acid as precursors, respectively, for the (R)-2-aza-3-chloro-β-tyrosine and the 2-naphthonate moieties in KED biosynthesis.

摘要

烯二炔天然产物的生物合成具有多条途径汇聚的特点,会生成独特的外围基团,这些基团连接在独特的烯二炔核心上。凯德菌素(KED)具有两个独特的外围基团,一个(R)-2-氮杂-3-氯-β-酪氨酸和一个带有异丙氧基的2-萘甲酸酯基团,以及两个脱氧糖。在凯德菌素中,这些外围基团与烯二炔核心的连接模式在立体化学构型方面与迄今为止研究的其他烯二炔不同。为了研究这些基团的生物合成并扩展我们对烯二炔核心形成的理解,从链霉菌属菌株ATCC 53650中克隆了凯德菌素的生物合成基因簇并进行了测序。对凯德菌素基因簇的生物信息学分析揭示了存在编码烯二炔核心生物合成的保守基因、可能负责2-氮杂-L-酪氨酸和3,6,8-三羟基-2-萘甲酸酯形成的I型和II型聚酮合酶基因座,以及已知参与脱氧糖生物合成的酶。凯德菌素基因簇中存在与负责来自C-1027和马杜霉素的L-酪氨酸衍生基团的生物合成、活化和偶联以及来自新制癌菌素的萘甲酸酯基团的生物合成、活化和偶联的基因同源的基因,分别支持2-氮杂-L-酪氨酸和3,6,8-三羟基-2-萘甲酸作为凯德菌素生物合成中(R)-2-氮杂-3-氯-β-酪氨酸和2-萘甲酸酯基团的前体。

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