胆盐出口泵
胆汁淤积
流出
肝细胞
多药耐药蛋白2
化学
小泡
生物化学
胆汁酸
运输机
体外
生物
ATP结合盒运输机
内分泌学
膜
基因
作者
Pieter Van Brantegem,Neel Deferm,Bing Qi,Tom De Vocht,Pieter Annaert
出处
期刊:Methods in molecular biology
日期:2019-01-01
卷期号:: 55-73
被引量:2
标识
DOI:10.1007/978-1-4939-9420-5_4
摘要
Transporters play a crucial role in the uptake of endo- and exogenous molecules in hepatocytes and efflux into the bile. The bile salt export pump (BSEP; ABCB11) is of major importance for efflux of bile salts to the bile and BSEP inhibition frequently provokes drug-induced cholestasis. This chapter describes two assays to determine inhibition of BSEP-mediated bile salt excretion. The first assay uses inside-out membrane vesicles, prepared from BSEP-transfected cell lines. The cholestasis potential of compounds can be determined by specifically investigating the ability to inhibit BSEP-mediated uptake of tauro-nor-THCA-24-DBD, a fluorescent bile salt derivative. For the second assay, relative accumulation of tauro-nor-THCA-24-DBD in sandwich-cultured hepatocytes, which represents a more biorelevant in vitro system, is investigated. Through incubation with standard or Ca2+/Mg2+-free buffer, the substrate signal can be determined in the cells and bile or the cells alone, respectively. Performing this assay in the presence and absence of potentially interfering compounds of interest enables exploration of the relative effect of these compounds on biliary excretion of the probe substrate.
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