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油酸对灌注大鼠肝脏中对硝基苯甲醚O-去甲基化的抑制作用。

Inhibition of p-nitroanisole O-demethylation in perfused rat liver by oleate.

作者信息

Danis M, Kauffman F C, Evans R K, Holtzclaw D, Reinke L A, Thurman R G

出版信息

Biochem Pharmacol. 1985 Mar 1;34(5):609-16. doi: 10.1016/0006-2952(85)90253-9.

Abstract

p-Nitroanisole O-demethylation in perfused livers from fasted, phenobarbital-treated rats was rapidly and reversibly inhibited by sodium oleate (0.3 to 0.6 mM). Xylitol partially reversed this inhibitory effect. The inhibition was not mediated by a direct effect of oleate on microsomal components since concentrations of oleate ranging up to 1.0 mM did not affect p-nitroanisole O-demethylation by isolated microsomes. Infusion of 0.6 mM oleate did not alter the measured intracellular NAD+/NADH ratio but did cause a significant increase in the intracellular NADP+/NADPH ratio. A significant decrease in the ATP/ADP ratio was also observed. Oleoyl CoA inhibited p-nitroanisole O-demethylation in microsomes (Ki about 30 microM), and both oleoyl CoA and palmitoyl CoA inhibited the energy-linked nicotinamide nucleotide transhydrogenase in submitochondrial particles (Ki about 1 microM). Thus, inhibition of mixed-function oxidation in the intact liver by oleate is most likely mediated by oleoyl CoA. Oleoyl CoA inhibits mixed-function oxidation in the intact liver by acting directly on cytochrome P-450 and by decreasing generation of NADPH via inhibition of key enzymes of the citric acid cycle and the energy-linked transhydrogenase.

摘要

在禁食且经苯巴比妥处理的大鼠的灌注肝脏中,油酸钠(0.3至0.6 mM)可快速且可逆地抑制对硝基苯甲醚O-去甲基化。木糖醇可部分逆转这种抑制作用。这种抑制并非由油酸对微粒体成分的直接作用介导,因为高达1.0 mM的油酸浓度并不影响分离出的微粒体对硝基苯甲醚的O-去甲基化。输注0.6 mM油酸不会改变所测得的细胞内NAD⁺/NADH比值,但会导致细胞内NADP⁺/NADPH比值显著升高。还观察到ATP/ADP比值显著降低。油酰辅酶A抑制微粒体中对硝基苯甲醚的O-去甲基化(Ki约为30 μM),油酰辅酶A和棕榈酰辅酶A均抑制亚线粒体颗粒中的能量偶联烟酰胺核苷酸转氢酶(Ki约为1 μM)。因此,油酸对完整肝脏中混合功能氧化的抑制很可能是由油酰辅酶A介导的。油酰辅酶A通过直接作用于细胞色素P-450并通过抑制柠檬酸循环的关键酶和能量偶联转氢酶来减少NADPH的生成,从而抑制完整肝脏中的混合功能氧化。

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