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Crystal Structures of Leukotriene C4 Synthase in Complex with Product Analogs

机译:白三烯C4合酶与产物类似物配合物的晶体结构

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摘要

Leukotriene (LT) C4 synthase (LTC4S) catalyzes the conjugation of the fatty acid LTA4 with the tripeptide GSH to produce LTC4, the parent compound of the cysteinyl leukotrienes, important mediators of asthma. Here we mutated Trp-116 in human LTC4S, a residue proposed to play a key role in substrate binding, into an Ala or Phe. Biochemical and structural characterization of these mutants along with crystal structures of the wild type and mutated enzymes in complex with three product analogs, viz. S-hexyl-, 4-phenyl-butyl-, and 2-hydroxy-4-phenyl-butyl-glutathione, provide new insights to binding of substrates and product, identify a new conformation of the GSH moiety at the active site, and suggest a route for product release, aided by Trp-116.
机译:白三烯(LT)C4合酶(LTC4S)催化脂肪酸LTA4与三肽GSH结合产生LTC4,LTC4是半胱氨酰白三烯的母体化合物,是哮喘的重要介体。在这里,我们将人LTC4S中的Trp-116突变为Ala或Phe,该残基被提议在底物结合中起关键作用。这些突变体的生化和结构表征,以及与三种产物类似物复合的野生型和突变酶的晶体结构。 S-己基-,4-苯基-丁基-和2-羟基-4-苯基-丁基-谷胱甘肽,提供了对底物和产物结合的新见解,在活性部位鉴定了GSH部分的新构象,并提出了建议Trp-116协助产品发布的途径。

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