Enterohepatic bile salt transporters in normal physiology and liver disease

胆盐出口泵 孕烷X受体 多药耐药蛋白2 肝肠循环 胆固醇7α羟化酶 胆汁酸 法尼甾体X受体 G蛋白偶联胆汁酸受体 CYP8B1 牛磺胆酸 小异二聚体伴侣 生物 ATP结合盒运输机 生物化学 化学 内科学 运输机 核受体 转录因子 基因 医学
作者
Gerd A. Kullak‐Ublick,Bruno Stieger,Peter J. Meier
出处
期刊:Gastroenterology [Elsevier BV]
卷期号:126 (1): 322-342 被引量:652
标识
DOI:10.1053/j.gastro.2003.06.005
摘要

Abstract

The vectorial transport of bile salts from blood into bile is essential for the generation of bile flow, solubilization of cholesterol in bile, and emulsification of lipids in the intestine. Major transport proteins involved in the enterohepatic circulation of bile salts include the hepatocellular bile salt export pump (BSEP, ABCB11), the apical sodium-dependent bile salt transporter (ASBT, SLC10A2) in cholangiocytes and enterocytes, the sodium-dependent hepatocyte bile salt uptake system NTCP (SLC10A1), the organic anion transporting polypeptides OATP-C (SLC21A6), OATP8 (SLC21A8) and OATP-A (SLC21A3), and the multidrug resistance protein MRP3 (ABCC3). Synthesis and transport of bile salts are intricately linked processes that undergo extensive feedback and feed-forward regulation by transcriptional and posttranscriptional mechanisms. A key regulator of hepatocellular bile salt homeostasis is the bile acid receptor/farnesoid X receptor FXR, which activates transcription of the BSEP and OATP8 genes and of the small heterodimer partner 1 (SHP). SHP is a transcriptional repressor that mediates bile acid-induced repression of the bile salt uptake systems rat Ntcp and human OATP-C. A nuclear receptor that activates rodent Oatp2 (Slc21a5) and human MRP2 (ABCC2) is the pregnane X receptor/steroid X receptor PXR/SXR. Intracellular trafficking and membrane insertion of bile salt transporters is regulated by lipid, protein, and extracellular signal-related kinases in response to physiologic stimuli such as cyclic adenosine monophosphate or taurocholate. Finally, dysfunction of individual bile salt transporters such as BSEP, on account of genetic mutations, steric inhibition, suppression of gene expression, or disturbed signaling, is an important cause of cholestatic liver disease.
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