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Expression of the platencin biosynthetic gene cluster in heterologous hosts yielding new platencin congeners

机译:产生新platencin同源异源宿主中的platencin生物合成基因簇的表达

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摘要

Platensimycin (PTM) and platencin (PTN) are potent and selective inhibitors of bacterial and mammalian fatty acid synthases and have emerged as promising drug leads for both antibacterial and antidiabetic therapies. We have previously cloned and sequenced the PTM-PTN dual biosynthetic gene cluster from S. platensis MA7327 and the PTN biosynthetic gene cluster from S. platensis MA7339, the latter of which is composed of 31 genes encoding PTN biosynthesis, regulation, and resistance. We have also demonstrated that PTM or PTN production can be significantly improved upon inactivation of the pathway specific regulator ptmR1 or ptnR1, in S. platensis MA7327 or MA7339, respectively. We now report engineered production of PTN and congeners in a heterologous Streptomyces host. Expression constructs containing the ptn biosynthetic gene cluster were engineered from SuperCos 1 library clones and introduced into five model Streptomyces hosts, and PTN production was achieved in Streptomyces lividans K4-114. Inactivation of ptnR1 was crucial for expression of the ptn biosynthetic gene cluster, thereby PTN production, in S. lividans K4-114. Six PTN congeners, five of which were new, were also isolated from the recombinant strain S. lividans SB12606, revealing new insights into PTN biosynthesis. Production of PTN in a model Streptomyces host provides new opportunities to apply combinatorial biosynthetic strategies to the PTN biosynthetic machinery for structural diversity.
机译:Platensimycin(PTM)和Platencin(PTN)是细菌和哺乳动物脂肪酸合酶的有效和选择性抑制剂,已成为抗菌和抗糖尿病治疗的有希望的药物先导。我们之前已经克隆和测序了来自链霉菌MA7327的PTM-PTN双生物合成基因簇和来自链霉菌MA7339的PTN生物合成基因簇,后者由31个编码PTN生物合成,调控和抗性的基因组成。我们还证明了,分别通过钝化链霉菌MA7327或MA7339中的途径特异性调节剂ptmR1或ptnR1灭活,可以显着提高PTM或PTN的产量。我们现在报告异源链霉菌宿主中PTN和同源物的工程化生产。从SuperCos 1文库克隆中工程改造了含有ptn生物合成基因簇的表达构建体,并将其构建到五种模型链霉菌宿主中,并在青链霉菌K4-114中实现了PTN的生产。 ptnR1的失活对于在li.S. lividans K4-114中ptn生物合成基因簇的表达,从而产生PTN至关重要。还从重组菌株S. lividans SB12606中分离了六个PTN同系物,其中五个是新的,揭示了对PTN生物合成的新见解。在模型链霉菌宿主中生产PTN提供了将组合生物合成策略应用于PTN生物合成机制以实现结构多样性的新机会。

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