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具有奇数双键的不饱和脂肪酸β-氧化的还原酶依赖性途径的意义。2-反式-5-顺式-辛二烯酰辅酶A的线粒体代谢。

Significance of the reductase-dependent pathway for the beta-oxidation of unsaturated fatty acids with odd-numbered double bonds. Mitochondrial metabolism of 2-trans-5-cis-octadienoyl-CoA.

作者信息

Shoukry K, Schulz H

机构信息

Department of Chemistry, City College, City University of New York, New York, New York 10031, USA.

出版信息

J Biol Chem. 1998 Mar 20;273(12):6892-9. doi: 10.1074/jbc.273.12.6892.

DOI:10.1074/jbc.273.12.6892
PMID:9506993
Abstract

The beta-oxidation of unsaturated fatty acids with odd-numbered double bonds proceeds by reduction of the double bond (reductase-dependent pathway) in addition to the well established isomerization of the double bond (isomerase-dependent pathway). The metabolic significance of the reductase-dependent pathway was assessed with 2-trans-5-cis-octadienoyl-CoA (2,5-octadienoyl-CoA) and its products, all of which are metabolites of alpha-linolenic acid. A kinetic evaluation of beta-oxidation enzymes revealed that the presence of a 5-cis double bond in the substrate most adversely affected the activity of 3-ketoacyl-CoA thiolase although not enough to become rate-limiting. Concentration-dependent and time-dependent measurements indicated that most (80%) of 2,5-octadienoyl-CoA is metabolized via the isomerase-dependent pathway. The reason for the greater flux through the isomerase-dependent pathway is the higher activity of L-3-hydroxyacyl-CoA dehydrogenase as compared with Delta3,Delta2-enoyl-CoA isomerase. These two enzymes catalyze the rate-limiting steps in the isomerase-dependent and reductase-dependent pathways, respectively. Once 2,5-octadienoyl-CoA is converted to 3,5-octadienoyl-CoA (perhaps fortuitously because of the presence of Delta3,Delta2-enoyl-CoA isomerase), the only effective route for its degradation is via the reductase-dependent pathway. It is concluded that the reductase-dependent pathway assures the degradation of 3,5-dienoyl-CoA intermediates, thereby preventing the depletion of free coenzyme A and a likely impairment of mitochondrial oxidative function.

摘要

除了已被充分证实的双键异构化(依赖异构酶途径)外,具有奇数双键的不饱和脂肪酸的β-氧化还通过双键还原(依赖还原酶途径)进行。利用2-反式-5-顺式-辛二烯酰辅酶A(2,5-辛二烯酰辅酶A)及其产物评估了依赖还原酶途径的代谢意义,所有这些都是α-亚麻酸的代谢产物。对β-氧化酶的动力学评估表明,底物中5-顺式双键的存在对3-酮酰辅酶A硫解酶的活性影响最大,尽管还不足以成为限速因素。浓度依赖性和时间依赖性测量表明,大多数(80%)的2,5-辛二烯酰辅酶A通过依赖异构酶途径代谢。通过依赖异构酶途径有更大通量的原因是与Δ3,Δ2-烯酰辅酶A异构酶相比,L-3-羟基酰基辅酶A脱氢酶的活性更高。这两种酶分别催化依赖异构酶途径和依赖还原酶途径中的限速步骤。一旦2,5-辛二烯酰辅酶A转化为3,5-辛二烯酰辅酶A(可能由于Δ3,Δ2-烯酰辅酶A异构酶的存在而偶然发生),其降解的唯一有效途径就是通过依赖还原酶途径。得出的结论是,依赖还原酶途径确保了3,5-二烯酰辅酶A中间体的降解,从而防止游离辅酶A的消耗以及可能的线粒体氧化功能损害。

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