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苯巴比妥对家兔甘油三酯代谢的影响。

Effects of phenobarbital upon triacylglycerol metabolism in the rabbit.

作者信息

Goldberg D M, Roomi M W, Yu A, Roncari D A

出版信息

Biochem J. 1980 Oct 15;192(1):165-75. doi: 10.1042/bj1920165.

Abstract
  1. The association between hepatic microsomal enzyme induction and triacylglycerol metabolism was examined in fasting male rabbits (2kg body wt.) injected intra-peritoneally with 50 mg of phenobarbital per kg for 10 days. 2. Occurrence of enzyme induction was established by a significant increase in hepatic aminopyrine N-demethylase activity and cytochrome P-450 content, as well as a doubling of microsomal protein per g of liver and a 54% increase in liver weight. Parallel increments in hepatic gamma-glutamyltransferase (EC 2.3.2.2) activity occurred; these were more pronounced in the whole homogenate than in the microsomes, which only accounted for 12.5% of the total enzyme activity in the controls and 17.0% in the animals given phenobarbital. Increased activity of gamma-glutamyltransferase activity was also observed in the blood serum of the test animals. 3. The rabbits given phenobarbital manifested increased hepatic triacylglycerol content and the triacylglycerol concentration of blood serum was also elevated. These changes were accompanied by a significantly enhanced ability of cell-free fractions of liver from the test animals (postmitochondrial supernatant and microsomal fractions) to synthesize glycerolipids in vitro from sn-[14C] glycerol 3-phosphate and fatty acids, when expressed per whole liver. Relative to the protein content of the fraction, glycerolipid synthesis in vitro was significantly decreased in the microsomes, presumably consequent upon the dramatic increase in their total protein content, whereas no change occurred in the postmitochondrial supernatant, possibly due to the protective effect of cytosolic factors present in this fraction and known to enhance glycerolipid synthesis. 4. Microsomal phosphatidate phosphohydrolase accounted for 85% of the total liver activity of this enzyme and its specific activity was 20-fold higher than that of the cytosolic phosphatidate phosphohydrolase (EC 3.1.3.4), when each was measured under optimal conditions. A significant increase in the activity of both enzymes per whole liver occurred in the rabbits given phenobarbital. A closer correlation between hepatic triacylglycerol content and and microsomal phosphatidate phosphohydrolase, as well as the above observation, suggest that this, rather than the cytosolic enzyme, may be rate-limiting for triacylglycerol synthesis in rabbit liver. 5. Significant correlations were observed between the various factors of hepatic microsomal-enzyme induction (aminopyrine N-demethylase and gamma-glutamyltransferase activity as well as cytochrome P-450 content) and hepatic triacylglycerol content, suggesting that that microsomal enzyme induction may promote hepatic triacylglycerol synthesis and consequently hypertriglyceridaemia in the rabbit.
摘要
  1. 在禁食的雄性家兔(体重2kg)中研究了肝微粒体酶诱导与三酰甘油代谢之间的关联,这些家兔腹腔注射每千克50mg苯巴比妥,持续10天。2. 通过肝氨基比林N-脱甲基酶活性、细胞色素P-450含量显著增加,以及每克肝脏微粒体蛋白加倍和肝脏重量增加54%来确定酶诱导的发生。肝脏γ-谷氨酰转移酶(EC 2.3.2.2)活性也有平行增加;这些在全匀浆中比在微粒体中更明显,微粒体中的酶活性在对照组中仅占总酶活性的12.5%,在给予苯巴比妥的动物中占17.0%。在试验动物的血清中也观察到γ-谷氨酰转移酶活性增加。3. 给予苯巴比妥的家兔肝脏三酰甘油含量增加,血清三酰甘油浓度也升高。这些变化伴随着试验动物肝脏的无细胞部分(线粒体后上清液和微粒体部分)从sn-[14C]甘油3-磷酸和脂肪酸体外合成甘油酯的能力显著增强,以全肝脏计算。相对于该部分的蛋白质含量,微粒体中的体外甘油酯合成显著降低,可能是由于其总蛋白质含量急剧增加,而线粒体后上清液中没有变化,可能是由于该部分中存在的细胞溶质因子的保护作用,已知该因子可增强甘油酯合成。4. 微粒体磷脂酸磷酸水解酶占该酶肝脏总活性的85%,在最佳条件下测量时,其比活性比细胞溶质磷脂酸磷酸水解酶(EC 3.1.3.4)高20倍。给予苯巴比妥的家兔每全肝脏中这两种酶的活性均显著增加。肝脏三酰甘油含量与微粒体磷脂酸磷酸水解酶之间的更紧密相关性,以及上述观察结果表明,可能是这种酶而不是细胞溶质酶对家兔肝脏中三酰甘油合成起限速作用。5. 在肝微粒体酶诱导的各种因素(氨基比林N-脱甲基酶和γ-谷氨酰转移酶活性以及细胞色素P-450含量)与肝脏三酰甘油含量之间观察到显著相关性,表明微粒体酶诱导可能促进家兔肝脏中三酰甘油合成,从而导致高甘油三酯血症。

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Effect of hydrazine exposure on hepatic triacylglycerol biosynthesis.肼暴露对肝脏三酰甘油生物合成的影响。
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本文引用的文献

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Stimulation of biosynthesis of glyceride.甘油酯生物合成的刺激作用。
Nature. 1967 Nov 4;216(5114):449-53. doi: 10.1038/216449a0.

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