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Probing the structure and function of acyl carrier proteins to unlock the strategic redesign of type II polyketide biosynthetic pathways

机译:探讨酰基载体蛋白的结构和功能解锁II型聚酮化合物生物合成途径的战略重新设计

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摘要

Type II polyketide synthases (PKSs) are protein assemblies, encoded by biosynthetic gene clusters in microorganisms, that manufacture structurally complex and pharmacologically relevant molecules. Acyl carrier proteins (ACPs) play a central role in biosynthesis by shuttling malonyl-based building blocks and polyketide intermediates to catalytic partners for chemical transformations. Because ACPs serve as central hubs in type II PKSs, they can also represent roadblocks to successfully engineering synthases capable of manufacturing ‘unnatural natural products.’ Therefore, understanding ACP conformational dynamics and protein interactions is essential to enable the strategic redesign of type II PKSs. However, the inherent flexibility and transience of ACP interactions pose challenges to gaining insight into ACP structure and function. In this review, we summarize how the application of chemical probes and molecular dynamic simulations has increased our understanding of the structure and function of type II PKS ACPs. We also share how integrating these advances in type II PKS ACP research with newfound access to key enzyme partners, such as the ketosynthase-chain length factor, sets the stage to unlock new biosynthetic potential.
机译:II型聚酮合成酶(PKS)是通过在微生物中的生物合成基因簇编码的蛋白质组件,其制造结构复杂和药理学相关分子。酰基载体蛋白(ACPs)通过穿梭基于丙基基层和聚酮化合物中间体对化学转化的催化作用,在生物合成中发挥着核心作用。由于ACPS作为II型PKS中的中央集线器,因此它们还可以代表成功化工合成能够制造“不自然产品”的障碍。因此,了解ACP构象动态和蛋白质相互作用对于实现II型PKSS的战略重新设计至关重要。然而,ACP交互的固有灵活性和特性构成了对ACP结构和功能洞察的挑战。在本综述中,我们总结了化学探针和分子动态模拟的应用如何增加了我们对II型PKS ACP的结构和功能的理解。我们还分享在II型PKS ACP研究中与关键酶合作伙伴(例如Ketosynthase-Chain Lengtom因子)的新进入集成这些进步如何设置阶段以解锁新的生物合成潜力。

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