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Analysis on the Substrate Specificity of Recombinant Human Acyl-CoA Synthetase ACSL4 Variants

机译:重组人酰基-CoA合成酶ACSL4变体的底物特异性分析

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Acyl-CoA synthetase long-chain family members (ACSLs) are a family of enzymes that convert long chain free fatty acids into their acyl-CoAs. ACSL4 is an ACSL isozyme with a strong preference for arachidonic acid (AA) and has been hypothesized to modulate the metabolic fates of AA. There are two ACSL4 splice variants: ACSL4V1, which is the more abundant transcript, and ACSL4V2, which is believed to be restricted to the brain. In the present study, we expressed recombinant human ACSL4V1 and V2 in Spodoptera frugiperda 9 (Sf9) cells using the baculovirus expression system and then partially purified both variants by cobalt affinity column chromatography. We then established a novel ACSL assay system with LC-MS/MS, which is highly sensitive and applicable to various kinds of fatty acids, and used it to investigate the substrate specificity of recombinant human ACSL4V1 and V2. The results showed that both ACSL4 variants preferred various kinds of highly unsaturated fatty acids (HUFAs), including docosahexaenoic acid (DHA), adrenic acid (docosatetraenoic acid) and eicosapentaenoic acid (EPA), as well as AA as a substrate. Moreover, our kinetic studies revealed that the two variants had similar relative affinities for AA, EPA and DHA but different reaction rates for each HUFA. These results confirmed the importance of both of ACSL4 variants in the maintenance of membrane phospholipids bearing HUFAs. Structural analysis of these variants might reveal the molecular mechanism by which they maintain membrane phospholipids bearing HUFAs.
机译:酰基-CoA合成酶的长链家族成员(ACSL)是一种酶系列,可将长链游离脂肪酸转化为其酰基-CoAs。 ACSL4是ACSL同工酶,其具有强烈偏好的花生素酸(AA),并已被假设以调节AA的代谢束。有两个ACSL4拼接变体:ACSL4V1,这是更丰富的转录物和ACSL4V2,据信限制为大脑。在本研究中,我们使用杆状病毒表达系统表达了烟草型塔蛋白酶的重组人ACSL4V1和V2,然后通过钴亲和柱色谱部分部分纯化了两种变体。然后,我们建立了一种具有LC-MS / MS的新型ACSL测定系统,其高度敏感和适用于各种脂肪酸,并使用它来研究重组人ACSL4V1和V2的底物特异性。结果表明,ACSL4变体均优选各种高度不饱和脂肪酸(HUFA),包括二十二碳六烯酸(DHA),肾上腺酸(DoCosateThoone酸)和己二辛烯酸(EPA),以及AA作为基质。此外,我们的动力学研究表明,两种变体对AA,EPA和DHA的相似性相似,但对于每种HUFA的不同反应速率。这些结果证实了ACSL4各种变体在轴承HUFA的膜磷脂中的重要性。这些变体的结构分析可能揭示它们维持携带HUFA的膜磷脂的分子机制。

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