4.6 Article

Monomeric bile acids modulate the ATPase activity of detergent-solubilized ABCB4/MDR3

期刊

JOURNAL OF LIPID RESEARCH
卷 62, 期 -, 页码 -

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ELSEVIER
DOI: 10.1016/j.jlr.2021.100087

关键词

ABC transporter; ABCB4/MDR3; bile acids; cholesterol; ATPase activity; TLCA; Nor-UDCA; critical micelle concentration

资金

  1. [CRC 974]

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ABCB4, also known as multidrug-resistant protein 3 (MDR3), is an ATP binding cassette transporter that specifically moves phosphatidylcholine (PC) lipids from the cytoplasmic to the extracellular leaflet in hepatocytes. Different bile acids can modulate its ATPase activity, with a nearly linear correlation between the critical micelle concentration and maximal stimulation by each bile acid. This study reveals the significant impact of 24-nor-ursodeoxycholic acid on ABCB4, suggesting a distinct regulation of ATPase activity compared to other bile acids.
ABCB4, also called multidrug-resistant protein 3 (MDR3), is an ATP binding cassette transporter located in the canalicular membrane of hepatocytes that specifically translocates phosphati dylcholine (PC) lipids from the cytoplasmic to the extracellular leaflet. Due to the harsh detergent effect of bile acids, PC lipids provided by ABCB4 are extracted into the bile. While it is well known that bile acids are the major extractor of PC lipids from the membrane into bile, it is unknown whether only PC lipid extraction is improved or whether bile acids also have a direct effect on ABCB4. Using in vitro experiments, we investigated the modulation of ATP hydrolysis of ABC by different bile acids commonly present in humans. We demonstrated that all tested bile acids stimulated ATPase activity except for taurolithocholic acid, which inhibited ATPase activity due to its hydrophobic nature. Additionally, we observed a nearly linear correlation between the critical micelle concentration and maximal stimulation by each bile acid, and that this modulation was maintained in the presence of PC lipids. This study revealed a large effect of 24-nor-ursodeoxycholic acid, suggesting a distinct mode of regulation of ATPase activity compared with other bile acids. In addition, it sheds light on the molecular cross talk of canalicular ABC transporters of the human liver.

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