首页> 美国卫生研究院文献>Biochemical Journal >Intramitochondrial control of the oxidation of hexadecanoate in skeletal muscle. A study of the acyl-CoA esters which accumulate during rat skeletal-muscle mitochondrial beta-oxidation of U-14Chexadecanoate and U-14Chexadecanoyl-carnitine.
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Intramitochondrial control of the oxidation of hexadecanoate in skeletal muscle. A study of the acyl-CoA esters which accumulate during rat skeletal-muscle mitochondrial beta-oxidation of U-14Chexadecanoate and U-14Chexadecanoyl-carnitine.

机译:骨骼肌中十六烷酸酯氧化的线粒体内控制。对在U-14C十六烷酸酯和U-14C十六烷酰肉碱的大鼠骨骼肌线粒体β-氧化过程中积累的酰基辅酶A酯的研究。

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摘要

1. We describe the acyl-CoA and acyl-carnitine esters which arise from the incubation of well-coupled State 3 rat skeletal-muscle mitochondrial fractions with [U-14C]hexadecanoate and [U-14C]hexadecanoyl-carnitine. 2. Acyl-CoA ester intermediates of chain length 16, 14, 12, 10 and 8 carbons were detected. 3. Although incubations were in steady state in respect of oxygen consumption, 14CO2 production and generation of acid-soluble radioactivity, quantitative analysis of acyl-CoA esters showed that steady state was not achieved in respect of all intermediates. 4. 3-Hydroxyacyl- and 2-enoyl-CoA and -carnitine esters were found under normoxic conditions. 5. Direct measurement of NAD+ and NADH shows that under identical incubation conditions our observations cannot be explained by gross perturbation of the [NAD+]/[NADH] ratio. 6. We hypothesize that there is a small pool of rapidly recycling NAD+ channelled between complex I of the respiratory chain and the newly described mitochondrial-inner-membrane-associated beta-oxidation trifunctional enzyme [Uchida, Izai, Orii and Hashimoto (1992) J. Biol. Chem. 267, 1034-1041].
机译:1.我们描述了酰基-CoA和酰基肉碱酯,它们是由状态良好的3号大鼠骨骼肌线粒体级分与[U-14C]十六烷酸酯和[U-14C]十六烷酰-肉碱共同孵育而成的。 2.检测到链长为16、14、12、10和8个碳的酰基-CoA酯中间体。 3.尽管在耗氧量,14CO2的产生和酸溶性放射性的产生方面处于稳定状态,但对酰基辅酶A酯的定量分析表明,并非所有中间体都达到稳定状态。 4.在常氧条件下发现了3-羟基-酰基和2-烯酰基-CoA和-肉碱酯。 5.对NAD +和NADH的直接测量表明,在相同的孵育条件下,[NAD +] / [NADH]比的总扰动无法解释我们的观察结果。 6.我们假设在呼吸链的复合体I与新描述的线粒体-内膜相关的β-氧化三功能酶之间存在一小部分快速循​​环的NAD +通道[Uchida,Izai,Orii和Hashimoto(1992)J生物学化学267,1034-1041]。

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