首页> 美国卫生研究院文献>Biochemical Journal >Effect of 25-hydroxycholesterol and bile acids on the regulation of cholesterol metabolism in Hep G2 cells.
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Effect of 25-hydroxycholesterol and bile acids on the regulation of cholesterol metabolism in Hep G2 cells.

机译:25-羟基胆固醇和胆汁酸对Hep G2细胞胆固醇代谢的调节作用。

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摘要

The effect of 25-hydroxycholesterol (25-OH-cholesterol) and chenodeoxycholic (CDC) acid on apoprotein secretion, low-density lipoprotein receptor activity, and [3H]triacylglycerol secretion in Hep G2 cells was studied. Both 25-OH-cholesterol and CDC acid increased the secretion of apolipoprotein (apo) E by Hep G2 cells. The secretion of apo A-I was slightly lowered (less than 10% disease). The maximal increase in apo E secretion was observed in culture medium containing 2 micrograms of 25-OH-cholesterol/ml or 10 micrograms of CDC acid/ml plus 10% fetal calf serum. Cholesterol, 7-OH-cholesterol and other bile acids were ineffective in inducing increases in apo E secretion. Another cholesterol synthesis inhibitor, mevinolin, was also ineffective in generating an increase in apoprotein secretion. The data indicated a specific interaction between 25-OH-cholesterol or CDC acid and apo E secretion in Hep G2 cells. Cholesterol synthesis, as measured by the incorporation of [14C]acetic acid into sterols, was repressed in Hep G2 cells in the presence of 25-OH-cholesterol (17% of control value). CDC acid, on the other hand, increased [14C]acetic acid incorporation (156% of control value). The number of LDL receptors in Hep G2 cells was decreased after incubation with 25-OH-cholesterol (62% of control value), but increased significantly after incubation with CDC acid (149% of control value). The secretion of [3H]triacylglycerol by Hep G2 cells incubated with 25-OH-cholesterol was greatly increased (248% of control value). On the contrary, CDC acid did not cause any increase in [3H]triacylglycerol secretion. The above results suggest that 25-OH-cholesterol and CDC acid have different effects on lipid metabolism in Hep G2 cells. The mRNA levels of apo E increased in cells preincubated with 25-OH-cholesterol and CDC acid, which suggested that the increase in apo E secretion is at least partly due to an increase in synthesis.
机译:研究了25-羟基胆固醇(25-OH-胆固醇)和鹅去氧胆酸(CDC)对Hep G2细胞中载脂蛋白分泌,低密度脂蛋白受体活性和[3H]三酰甘油分泌的影响。 25-OH-胆固醇和CDC酸均可增加Hep G2细胞分泌载脂蛋白(apo)E的能力。载脂蛋白A-I的分泌略有降低(疾病少于10%)。在含有2微克25-OH-胆固醇/ ml或10微克CDC酸/ ml加10%胎牛血清的培养基中观察到apo E分泌的最大增加。胆固醇,7-OH-胆固醇和其他胆汁酸在诱导Apo E分泌增加方面无效。另一种胆固醇合成抑制剂美维诺林,在载脂蛋白分泌增加方面也无效。数据表明Hep G2细胞中25-OH-胆固醇或CDC酸与载脂蛋白E分泌之间存在特异性相互作用。在25-OH-胆固醇存在下(在控制值的17%的情况下),在Hep G2细胞中抑制了胆固醇合成(通过将[14C]乙酸掺入甾醇中来测量)。另一方面,CDC酸可增加[14C]乙酸的掺入(控制值的156%)。用25-OH-胆固醇孵育后,Hep G2细胞中LDL受体的数量减少(占对照值的62%),但与CDC酸孵育后,LDL受体的数量显着增加(对照值的149%)。与25-OH-胆固醇一起孵育的Hep G2细胞分泌的[3H]三酰基甘油大大增加(控制值的248%)。相反,CDC酸并未引起[3H]三酰基甘油分泌的增加。上述结果表明25-OH-胆固醇和CDC酸对Hep G2细胞中脂质代谢的影响不同。在用25-OH-胆固醇和CDC酸预孵育的细胞中,载脂蛋白E的mRNA水平增加,这表明载脂蛋白E分泌的增加至少部分是由于合成的增加。

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