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Discovery of a new peptide natural product by Streptomyces coelicolor genome mining

机译:通过天蓝色链霉菌基因组挖掘发现一种新的肽天然产物

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Analyses of microbial genome sequences reveal numerous examples of gene clusters encoding proteins typically involved in complex natural product biosynthesis but not associated with the production of known natural products1"3. In Streptomyces coelicolor M145 there are several gene clusters encoding new nonribosomal peptide synthetase (NRPS) systems not associated with known metabolites. Application of structure-based models for substrate recognition by NRPS adenylation domains4"6 predicts the amino acids incorporated into the putative peptide products of these systems7'3, but the accuracy of these predictions is untested. Here we report the isolation and structure determination of the new tris-hydroxamate tetrapeptide iron chelator coelichelin from S. coelicolor using a genome mining approach guided by substrate predictions for the trimodular NRPS CchH, and we show that this enzyme, which lacks a C-terminal thioesterase domain, together with a homolog of enterobactin esterase (CchJ), are required for coelichelin biosynthesis. These results demonstrate that accurate prediction of adenylation domain substrate selectivity is possible and raise intriguing mechanistic questions regarding the assembly of a tetrapeptide by a trimodular NRPS.
机译:微生物基因组序列分析揭示了许多编码通常参与复杂的天然产物生物合成但与已知天然产物的生产无关的蛋白质的基因簇的例子。在天蓝色链霉菌M145中,有几个编码新的非核糖体肽合成酶(NRPS)的基因簇NRPS腺苷酸化域4“ 6的底物识别基于结构的模型的应用预测了掺入这些系统推定的肽产物中的氨基酸7'3,但是这些预测的准确性尚未得到检验。在这里,我们报告了一种新的三异羟肟酸酯四肽铁螯合剂coelichelin的分离和结构测定,该酶是利用三基团NRPS CchH的底物预测指导的基因组挖掘方法从基因组挖掘方法中获得的,并且我们证明了这种缺乏C末端的酶鹅肠素生物合成需要硫酯酶结构域和肠杆菌素酯酶(CchJ)的同源物。这些结果表明,对腺苷酸化域底物选择性的准确预测是可能的,并且提出了关于通过三模块NRPS组装四肽的有趣的机械问题。

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