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地塞米松和亚油酸对胆汁脂质及阴离子多肽因子肝分泌的影响:体内和体外研究

Effects of dexamethasone and linoleic acid on hepatic secretion of biliary lipids and anionic polypeptide factor: In vivo and in vitro studies.

作者信息

Domingo N, Debono E, Reynier M O, Crotte C, Thorin B, Charbonnier M, Clerc T, Grillasca J, Chanussot F, Lafont H

机构信息

U476-Inserm, Viton Center, Marseilles, France.

出版信息

Digestion. 1999 Nov-Dec;60(6):515-21. doi: 10.1159/000007700.

Abstract

Synthetic glucocorticoids, such as dexamethasone, and diets enriched with unsaturated fatty acids have been shown to stimulate hepatic bile salt synthesis. This fact led us to investigate the effects of dexamethasone and linoleic acid supplementation on bile secretion. Cholesterol (Ch) and phospholipid secretions are bile acid dependent. Ch and phospholipid in bile are also highly bound to a small apoprotein, the anionic polypeptide factor (APF). In bile, APF may play a physiological role in stabilizing cholesterol:phospholipid vesicles and might also be important in the regulatory process of bile lipid secretion. In order to study the factors influencing bile secretion, the biliary secretion rates of bile lipids and APF were experimentally modulated in perfused rat liver (PRL) and HepG2 cells. As expected, dexamethasone induced an increase in the biliary secretion rate of bile salts (BS) in the two models (PRL: 34 up to 67 nmol/l/min/g liver; HepG2 cells: 234% vs. 100% in controls). The bile secretion rates for phospholipids (PRL: from 5 down to 1.5 nmol/l/min/g liver; HepG2 cells: 93 vs. 100% in controls) and APF (PRL: from 0.34 down to 0.12 microg/l/min/g liver; cells: 86 vs. 100% in controls) rapidly decreased independently from those of BS. The data from experimental cell models supplemented with linoleic acid indicated a correlation between the BS and APF levels (APF: 71 and 63%; BS: 161 and 197% vs. 100% in controls). The phospholipid level was regulated independently from that of APF and BS and increased (106 and 111% vs. 100% in controls), while Ch remained nevertheless unchanged. Our data showed that dexamethasone induced changes in bile and that linoleic acid clearly impaired the regulation exerted by the dexamethasone on bile lipids.

摘要

已表明,合成糖皮质激素(如地塞米松)以及富含不饱和脂肪酸的饮食可刺激肝脏胆汁盐的合成。这一事实促使我们研究地塞米松和补充亚油酸对胆汁分泌的影响。胆固醇(Ch)和磷脂的分泌依赖于胆汁酸。胆汁中的Ch和磷脂也与一种小载脂蛋白——阴离子多肽因子(APF)高度结合。在胆汁中,APF可能在稳定胆固醇:磷脂囊泡方面发挥生理作用,并且在胆汁脂质分泌的调节过程中可能也很重要。为了研究影响胆汁分泌的因素,在灌注大鼠肝脏(PRL)和HepG2细胞中对胆汁脂质和APF的胆汁分泌速率进行了实验性调节。正如预期的那样,地塞米松在两种模型中均诱导胆汁盐(BS)的胆汁分泌速率增加(PRL:从34增加至67 nmol/升/分钟/克肝脏;HepG2细胞:相对于对照组的100%,增加至234%)。磷脂的胆汁分泌速率(PRL:从5降至1.5 nmol/升/分钟/克肝脏;HepG2细胞:相对于对照组的100%,为93%)和APF的胆汁分泌速率(PRL:从0.34降至0.12微克/升/分钟/克肝脏;细胞:相对于对照组的100%,为86%)与BS的分泌速率无关,迅速下降。补充亚油酸的实验细胞模型的数据表明BS和APF水平之间存在相关性(APF:相对于对照组的100%,分别为71%和63%;BS:分别为161%和197%)。磷脂水平的调节独立于APF和BS,且有所增加(相对于对照组的100%,分别为106%和111%),而Ch水平则保持不变。我们的数据表明,地塞米松会引起胆汁变化,并且亚油酸明显削弱了地塞米松对胆汁脂质的调节作用。

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