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Unconventional origin and hybrid system for construction of pyrrolopyrrole moiety in kosinostatin biosynthesis

机译:非传统起源和杂交体系在kosinostatin生物合成中构建吡咯并吡咯部分

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Summary Kosinostatin (KST), an antitumor antibiotic, features a pyrrolopyrrole moiety spirally jointed to a five-membered ring of an anthraquinone framework glycosylated with a γ-branched octose. By a combination of in silico analysis, genetic characterization, biochemical assay, and precursor feeding experiments, a biosynthetic pathway for KST was proposed, which revealed (1) the pyrrolopyrrole moiety originates from nicotinic acid and ribose, (2) the bicyclic amidine is constructed by a process similar to the tryptophan biosynthetic pathway, and (3) a discrete adenylation enzyme and a peptidyl carrier protein (PCP) are responsible for producing a PCP-tethered building block parallel to type II polyketide synthase (PKS) rather than for the PKS priming step by providing the starter unit. These findings provide an opportunity to further explore the inexplicable enzymatic logic that governs the formation of pyrrolopyrrole moiety and the spirocyclic skeleton.
机译:概述抗肿瘤抗生素科西汀汀(KST)的特征是吡咯并吡咯部分螺旋连接到被γ-支链八糖糖基化的蒽醌骨架的五元环上。通过计算机分析,遗传表征,生化测定和前体进料实验相结合,提出了KST的生物合成途径,揭示了(1)吡咯并吡咯部分来源于烟酸和核糖,(2)构建了双环am (3)离散的腺苷酸化酶和肽基载体蛋白(PCP)负责产生与II型聚酮化合物合酶(PKS)平行的PCP束缚结构单元,而不是PKS通过提供起动器单元进行灌注步骤。这些发现提供了进一步探索控制吡咯并吡咯部分和螺环骨架形成的莫名其妙的酶学逻辑的机会。

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