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首页> 外文期刊>Environmental microbiology >Biosynthesis of the antifungal haterumalide, oocydin A, in Serratia, and its regulation by quorum sensing, RpoS and Hfq
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Biosynthesis of the antifungal haterumalide, oocydin A, in Serratia, and its regulation by quorum sensing, RpoS and Hfq

机译:沙雷氏菌中的抗真菌合剂灵芝内酯oocydin A的生物合成及其通过群体感应,RpoS和Hfq的调控

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摘要

Polyketides represent an important class of bioactive natural products with a broad range of biological activities. We identified recently a large trans-acyltransferase (AT) polyketide synthase gene cluster responsible for the biosynthesis of the antifungal, anti-oomycete and antitumor haterumalide, oocydin A (ooc). Using genome sequencing and comparative genomics, we show that the ooc gene cluster is widespread within biocontrol and phytopathogenic strains of the enterobacteria, Serratia and Dickeya. The analysis of in frame deletion mutants confirmed the role of a hydroxymethylglutaryl-coenzyme A synthase cassette, three flavin-dependent tailoring enzymes, a free-standing acyl carrier protein and two hypothetical proteins in oocydin A biosynthesis. The requirement of the three trans-acting AT domains for the biosynthesis of the macrolide was also demonstrated. Expression of the ooc gene cluster was shown to be positively regulated by an N-acyl-L-homoserine lactone-based quorum sensing system, but operating in a strain-dependent manner. At a post-transcriptional level, the RNA chaperone, Hfq, plays a key role in oocydin A biosynthesis. The Hfq-dependent regulation is partially mediated by the stationary phase sigma factor, RpoS, which was also shown to positively regulate the synthesis of the macrolide. Our results reveal differential regulation of the divergently transcribed ooc transcriptional units, highlighting the complexity of oocydin A production.
机译:聚酮化合物代表了一类重要的生物活性天然产物,具有广泛的生物活性。我们最近确定了一个大型的反式酰基转移酶(AT)聚酮化合物合酶基因簇,负责抗真菌,抗卵菌和抗肿瘤的Haterumalide,卵磷脂A(ooc)的生物合成。使用基因组测序和比较基因组学,我们表明,ooc基因簇广泛存在于肠杆菌,沙雷氏菌和迪卡菌的生物防治和植物致病菌株中。框内缺失突变体的分析证实了卵磷脂A生物合成中羟甲基戊二酰辅酶A合酶盒,三种黄素依赖性剪裁酶,独立式酰基载体蛋白和两种假设蛋白的作用。还证明了三个反式作用的AT结构域对大环内酯生物合成的需求。已显示,ooc基因簇的表达受基于N-酰基-L-高丝氨酸内酯的群体感应系统的正调控,但以依赖菌株的方式运行。在转录后水平上,RNA伴侣Hfq在卵磷脂A生物合成中起关键作用。 Hfq依赖的调节部分由固定相西格玛因子RpoS介导,该因子也显示出正调控大环内酯的合成。我们的结果揭示了不同转录的ooc转录单位的差异调节,突显了卵磷脂A产生的复杂性。

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