首页> 美国卫生研究院文献>Biochemical Journal >Contribution of newly synthesized cholesterol to rat plasma and bile determined by mass isotopomer distribution analysis: bile-salt flux promotes secretion of newly synthesized cholesterol into bile.
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Contribution of newly synthesized cholesterol to rat plasma and bile determined by mass isotopomer distribution analysis: bile-salt flux promotes secretion of newly synthesized cholesterol into bile.

机译:通过质量同位素异构体分布分析确定了新合成的胆固醇对大鼠血浆和胆汁的贡献:胆盐通量促进了新合成的胆固醇向胆汁的分泌。

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摘要

To quantify the contribution of newly synthesized cholesterol to total plasma and biliary cholesterol under physiological conditions, unrestrained rats were infused intravenously with [1-13C]acetate (0. 6mmol/h per kg) from 12:00 to 24:00 h, and fractional and absolute cholesterol-synthesis rates were determined by mass isotopomer distribution analysis (MIDA). As bile diversion leads to changes in cholesterol metabolism, rats were equipped with permanent catheters in the bile duct and duodenum, allowing sampling of small amounts of bile from an intact enterohepatic circulation. For comparison, rats with chronic bile diversion were also studied. Fractional synthesis of plasma cholesterol was 10.8+/-1.7% (mean+/-S.D.) after 12 h in rats with intact circulation. Fractional synthesis of biliary cholesterol was significantly higher than that of plasma cholesterol, i.e. 16.5+/-2.0% (P<0.05) after 12 h. In contrast, no differences between fractional synthesis of cholesterol in plasma and bile were found in bile-diverted animals (31.8+/-2.1 and 33.1+/-3.3% respectively after 12 h). The calculated absolute rate of cholesterol biosynthesis increased from 53+/-10 to 221+/-19 micromol/day per kg after bile diversion. A comparison of MIDA results with those obtained from balance studies indicated that MIDA does not assess total body synthesis in rats, presumably because of incomplete equilibration of newly synthesized molecules with cholesterol in the plasma compartment. These studies demonstrate that the contribution of newly synthesized cholesterol to biliary cholesterol is higher than to plasma cholesterol under physiological conditions, probably reflecting bile-salt-induced secretion of newly formed cholesterol by the periportal hepatocytes.
机译:为了量化在生理条件下新合成的胆固醇对总血浆和胆汁胆固醇的贡献,在12:00至24:00时向未受限制的大鼠静脉内注入[1-13C]乙酸盐(0. 6mmol / h / kg),并通过质量同位素异构体分布分析(MIDA)确定胆固醇的分数和绝对合成速率。由于胆汁转移导致胆固醇代谢改变,因此大鼠在胆管和十二指肠中配备了永久性导管,从而可以从完整的肝肠循环中提取少量胆汁。为了进行比较,还研究了具有慢性胆汁转移的大鼠。在完整循环的大鼠中,血浆胆固醇在12小时后的分数合成为10.8 +/- 1.7%(平均值+/-标准差)。胆汁胆固醇的分数合成显着高于血浆胆固醇,即12小时后为16.5 +/- 2.0%(P <0.05)。相反,在胆汁转移的动物中,血浆和胆汁中胆固醇的分数合成之间没有差异(12小时后分别为31.8 +/- 2.1和33.1 +/- 3.3%)。胆汁转移后,胆固醇的生物合成绝对速率从每公斤53 +/- 10微克/天增加到221 +/- 19微摩尔/天。将MIDA结果与从平衡研究中获得的结果进行比较表明,MIDA不能评估大鼠体内的整体合成,大概是因为新合成的分子与血浆室内胆固醇的不完全平衡。这些研究表明,在生理条件下,新合成的胆固醇对胆汁胆固醇的贡献高于对血浆胆固醇的贡献,这可能反映了胆盐诱导的门静脉肝细胞分泌新形成的胆固醇。

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