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Biochemical and Structural Characterization of Germicidin Synthase: Analysis of a Type III Polyketide Synthase that Employs Acyl-ACP as a Starter Unit Donor

机译:杀菌素合成酶的生化和结构表征:A III型聚酮合成酶的分析其采用酰基-ACP作为起动器单元供体

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摘要

Germicidin synthase (Gcs) from Streptomyces coelicolor is a type III polyketide synthase (PKS) with broad substrate flexibility for acyl groups linked through a thioester bond to either coenzyme A (CoA) or acyl carrier protein (ACP). Germicidin synthesis was reconstituted in vitro by coupling Gcs with fatty acid biosynthesis. Since Gcs has broad substrate flexibility, we directly compared the kinetic properties of Gcs with both acyl-ACP and acyl-CoA. The catalytic efficiency of Gcs for acyl-ACP was 10-fold higher than for acyl-CoA suggesting a strong preference towards carrier protein starter unit transfer. The 2.9 Å germicidin synthase crystal structure revealed canonical type III PKS architecture along with an unusual helical bundle of unknown function that appears to extend the dimerization interface. A pair of arginine residues adjacent to the active site affect catalytic activity but not ACP binding. This investigation provides new and surprising information about the interactions between type III PKSs and ACPs that will facilitate the construction of engineered systems for production of novel polyketides.
机译:来自链霉菌的杀菌素合酶(GCS)是一种III型聚酮合成酶(PKS),其具有宽的基材柔韧性,用于连接通过硫酯键与辅酶A(COA)或酰基载体蛋白(ACP)连接的酰基。通过将GCS与脂肪酸生物合成偶联,体外重构杀菌蛋白合成。由于GCS具有宽的基材灵活性,因此我们将GCS的动力学与酰基-ACP和酰基-COA进行了直接比较了GCS的动力学性质。酰基-ACP的GCS的催化效率高于酰基-CoA的10倍,表明对载体蛋白启动单元转移的强偏好。 2.9Å杀菌素合成酶晶体结构揭示了规范型III PKS架构以及一个不寻常的未知功能的螺旋束,似乎延长了二聚化界面。与活性位点相邻的一对精氨酸残基会影响催化活性但不是ACP结合。本调查提供了有关III型PKSS和ACPS之间的相互作用的新信息,可促进用于生产新型聚酮化合物的工程系统。

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