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ATP8B1和ATP11C:对肝细胞功能至关重要的两种脂质翻转酶。

ATP8B1 and ATP11C: Two Lipid Flippases Important for Hepatocyte Function.

作者信息

Naik Jyoti, de Waart Dirk R, Utsunomiya Karina, Duijst Suzanne, Mok Kam Ho, Oude Elferink Ronald P J, Bosma Piter J, Paulusma Coen C

机构信息

Academic Medical Center, Tytgat Institute for Liver and Intestinal Research, Amsterdam, The Netherlands.

出版信息

Dig Dis. 2015;33(3):314-8. doi: 10.1159/000371665. Epub 2015 May 27.

Abstract

P4 ATPases are lipid flippases and transport phospholipids from the exoplasmic to the cytosolic leaflet of biological membranes. Lipid flipping is important for the biogenesis of transport vesicles. Recently it was shown that loss of the P4 ATPases ATP8B1 and ATP11C are associated with severe Cholestatic liver disease. Mutation of ATP8B1 cause progressive familial Intrahepatic Cholestasis type 1 (PFIC1)and benign recurrent intrahepatic cholestasis type 1 (BRIC 1). From our observations we hypothesized that ATP8B1 deficiency causes a phospholipids randomization at the canalicular membrane, which results in extraction of cholesterol due to increase sensitivity of the canalicular membrane. Deficiency of ATP11C causes conjugated hyperbilirubinemia. In our preliminary result we observed accumulation of unconjugated bile salts in Atp11c deficient mice probably because of regulation in the expression or function of OATP1B2. Similar to ATP8B1, ATP11C have regulation on membrane transporters.

摘要

P4 ATP酶是脂质翻转酶,可将磷脂从生物膜的细胞外小叶转运至胞质小叶。脂质翻转对于运输小泡的生物发生很重要。最近研究表明,P4 ATP酶ATP8B1和ATP11C的缺失与严重的胆汁淤积性肝病有关。ATP8B1的突变会导致1型进行性家族性肝内胆汁淤积症(PFIC1)和1型良性复发性肝内胆汁淤积症(BRIC 1)。根据我们的观察,我们推测ATP8B1缺乏会导致胆小管膜处的磷脂随机化,这会由于胆小管膜敏感性增加而导致胆固醇的提取。ATP11C缺乏会导致结合型高胆红素血症。在我们的初步结果中,我们观察到Atp11c缺陷小鼠中未结合胆汁盐的积累,这可能是由于OATP1B2的表达或功能受到调节。与ATP8B1类似,ATP11C对膜转运蛋白也有调节作用。

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