消胆胺对人体服用熊去氧胆酸期间胆汁酸模式及合成的影响。

Effect of cholestyramine on bile acid pattern and synthesis during administration of ursodeoxycholic acid in man.

作者信息

Rust C, Sauter G H, Oswald M, Büttner J, Kullak-Ublick G A, Paumgartner G, Beuers U

机构信息

Department of Medicine II, University of Munich, Germany.

出版信息

Eur J Clin Invest. 2000 Feb;30(2):135-9. doi: 10.1046/j.1365-2362.2000.00606.x.

DOI:10.1046/j.1365-2362.2000.00606.x

PMID:10651838

Abstract

BACKGROUND

Cholestyramine is the first-line treatment for cholestasis-induced pruritus and is prescribed along with ursodeoxycholic acid (UDCA) in patients with cholestatic liver diseases. Impairment of the intestinal absorption of endogenous hydrophobic bile acids by cholestyramine is well known. It is unclear, however, whether cholestyramine also impairs the absorption of the hydrophilic bile acid, UDCA, in man.

AIMS

To study serum levels of UDCA and endogenous bile acids as well as endogenous bile acid synthesis during simultaneous or separate administration of UDCA and cholestyramine in vivo; and absorption of UDCA both in the presence and absence of its hydrophobic epimer, chenodeoxycholic acid (CDCA), by cholestyramine in vitro.

PATIENTS AND METHODS

Five healthy subjects received UDCA (12.5 +/- 0.5 mg kg-1 daily) as a single dose for periods of 14 days with or without cholestyramine (4 g daily). Fasting serum levels of bile acids and of 7alpha-hydroxy-4-cholesten-3-one (alpha-HC), a measure of endogenous bile acid synthesis, were determined by gas chromatography and high pressure liquid chromatography, respectively. In vitro, bile acid solutions were incubated for 24 h in the presence or absence of cholestyramine, and bile acid concentrations were determined in the supernatant.

RESULTS

Simultaneous administration of UDCA and cholestyramine in man led to a decrease of fasting serum levels of UDCA by 60% when compared to UDCA serum levels during administration of UDCA alone. In contrast, serum levels of endogenous bile acids were not affected and alpha-HC serum levels were found increased 2. 7-fold indicating stimulation of endogenous bile acid synthesis by cholestyramine. Administration of cholestyramine and UDCA at an interval of 5 h tended to diminish the effect of cholestyramine on UDCA serum levels. In vitro, conjugated and unconjugated UDCA were effectively bound by cholestyramine both in the presence and absence of hydrophobic bile acids.

CONCLUSIONS

The results strongly support the recommendation to administer UDCA and cholestyramine at different times of day.

摘要

背景

考来烯胺是胆汁淤积性瘙痒的一线治疗药物，在胆汁淤积性肝病患者中与熊去氧胆酸（UDCA）联合使用。考来烯胺对内源性疏水胆汁酸肠道吸收的损害是众所周知的。然而，考来烯胺是否也会损害人体内亲水性胆汁酸UDCA的吸收尚不清楚。

目的

研究在体内同时或分别给予UDCA和考来烯胺时UDCA和内源性胆汁酸的血清水平以及内源性胆汁酸的合成；并在体外研究考来烯胺在有或没有其疏水差向异构体鹅去氧胆酸（CDCA）存在的情况下对UDCA的吸收情况。

患者和方法

五名健康受试者接受UDCA（每日12.5±0.5mg/kg）单剂量给药，为期14天，期间有或没有考来烯胺（每日4g）。空腹血清胆汁酸水平和7α-羟基-4-胆甾烯-3-酮（α-HC）（内源性胆汁酸合成的一项指标）分别通过气相色谱法和高压液相色谱法测定。在体外，胆汁酸溶液在有或没有考来烯胺的情况下孵育24小时，并测定上清液中的胆汁酸浓度。

结果

与单独给予UDCA期间的UDCA血清水平相比，人体内同时给予UDCA和考来烯胺导致空腹血清UDCA水平降低60%。相比之下，内源性胆汁酸的血清水平未受影响，而α-HC血清水平升高了2.7倍，表明考来烯胺刺激了内源性胆汁酸的合成。考来烯胺和UDCA间隔5小时给药倾向于减少考来烯胺对UDCA血清水平的影响。在体外，无论有无疏水胆汁酸存在，结合型和非结合型UDCA均能被考来烯胺有效结合。