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Loading of malonyl-CoA onto tandem acyl carrier protein domains of polyunsaturated fatty acid synthases

机译:丙二酰辅酶A加载到多不饱和脂肪酸合成酶的串联酰基载体蛋白结构域上

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摘要

Omega-3 polyunsaturated fatty acids (PUFA) are produced in some unicellular organisms, such as marine gammaproteobacteria, myxobacteria, and thraustochytrids, by large enzyme complexes called PUFA synthases. These enzymatic complexes resemble bacterial antibiotic-producing proteins known as polyketide synthases (PKS). One of the PUFA synthase subunits is a conserved large protein (PfaA in marine proteobacteria) that contains three to nine tandem acyl carrier protein (ACP) domains as well as condensation and modification domains. In this work, a study of the PfaA architecture and its ability to initiate the synthesis by selecting malonyl units has been carried out. As a result, we have observed a self-acylation ability in tandem ACPs whose biochemical mechanism differ from the previously described for type II PKS. The acyltransferase domain of PfaA showed a high selectivity for malonyl-CoA that efficiently loads onto the ACPs domains. These results, together with the structural organization predicted for PfaA, suggest that this protein plays a key role at early stages of the anaerobic pathway of PUFA synthesis.
机译:Omega-3多不饱和脂肪酸(PUFA)是通过称为PUFA合酶的大型酶复合物在某些单细胞生物中产生的,例如海洋γ-变形杆菌,粘细菌和破囊壶菌。这些酶复合物类似于被称为聚酮化合物合酶(PKS)的细菌产生抗生素的蛋白质。 PUFA合酶亚基之一是保守的大蛋白(海洋蛋白细菌中为PfaA),其中包含三到九个串联酰基载体蛋白(ACP)域以及缩合和修饰域。在这项工作中,已经进行了PfaA结构及其通过选择丙二酰单元引发合成的能力的研究。结果,我们观察到了串联ACP的自酰化能力,其生化机制与先前描述的II型PKS不同。 PfaA的酰基转移酶结构域显示出对丙二酰辅酶A的高选择性,可有效加载到ACPs域上。这些结果,以及为PfaA预测的结构组织,表明该蛋白在PUFA合成厌氧途径的早期阶段起着关键作用。

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