首页> 外文期刊>Molecular pharmaceutics >ATP-Binding Cassette Transporter A Subfamily 8 Is a Sinusoidal Efflux Transporter for Cholesterol and Taurocholate in Mouse and Human Liver
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ATP-Binding Cassette Transporter A Subfamily 8 Is a Sinusoidal Efflux Transporter for Cholesterol and Taurocholate in Mouse and Human Liver

机译:ATP结合盒式磁带转运蛋白8是用于胆固醇和牛磺酸的小鼠和人肝脏的正弦流动转运蛋白

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摘要

The ATP-binding cassette (ABC) transporter A subfamily 8 (ABCA8) belongs to the ABCA6-like transporters subgroup, which is distinct from the ABCA1-like subgroup in the ABCA family. The expression and function of the short-size human ABCA8 lacking one of the two ATP-binding domains for ATP hydrolysis, which are regularly present in the other ABCA transporters, have been reported. However, the functional differences between the short-size human ABCA8 and full-size human ABCA8, which has the two ATP-binding domains, remain unknown. The purpose of the present study was to clarify the tissue expression profiles of ABCA6-like and ABCA1-like subgroup transporters and the functional characteristics of ABCA8 in mouse and human. The tissue distribution of mouse ABCA (mABCA) transporter protein and the changes in mABCA8 protein expression levels in a mouse model of obstructive cholestasis were elucidated by means of quantitative targeted absolute proteomics (QTAP). The transport characteristics were clarified in a HEK293 cell line overexpressing full-size ABCA8 protein. QTAP and immunohistochemical analyses revealed that mABCA transporters exhibited the distinct protein expression patterns in the tissues, and mABCA8b, its mouse orthologue, was abundant in the liver and predominantly distributed in sinusoidal membranes of the hepatocytes. Further, protein expression of mABCA8b was decreased in the mouse cholestasis liver. Changes of mABCA8b expression level in cholestasis were similar to those of mABCA1, a sinusoidal cholesterol efflux transporter. Uptake and efflux assays showed that ABCA8 mediates efflux of [~(3)H]cholesterol and [~(3)H]taurocholate, while it showed no significant efflux activity for [~(3)H]estrone sulfate, [~(3)H]digoxin, [~(3)H]vinblastine, [~(3)H] para -aminohippuric acid, [~(3)H]oleic acid, [~(14)C]nicotine, or [~(3)H]methotrexate. [~(3)H]Cholesterol efflux was increased by extracellularly applied taurocholate. These results suggest that mABCA8b/ABCA8 functions as a sinusoidal efflux transporter for at least cholesterol and taurocholate in mouse and human liver.
机译:ATP结合盒(ABC)转运蛋白是亚家族8(ABCA8)属于ABCA6样的转运蛋白组,其与ABCA系列中的ABCA1样亚组不同。据报道,缺少用于ATP水解的两种ATP结合结构域之一的短尺寸人ABCA8的表达和功能,其定期存在于其他ABCA转运蛋白中。然而,短尺寸人体ABCA8和具有两个ATP结合结构域的全尺寸人ABCA8之间的功能差异仍然未知。本研究的目的是阐明ABCA6样和ABCA1样亚组转运蛋白的组织表达谱和小鼠和人中ABCA8的功能特征。通过定量靶向绝对蛋白质组学(QTAP)阐明了小鼠ABCA(MABCA)转运蛋白的组织分布和MABCA8蛋白表达水平的MABCA8蛋白表达水平的变化。在过表达全尺寸ABCA8蛋白的HEK293细胞系中澄清了传输特性。 QTAP和免疫组织化学分析显示,MABCA转运蛋白在组织中表现出不同的蛋白质表达模式,并且MABCA8B,其小鼠直晶型在肝脏中丰富,主要分布在肝细胞的正弦膜中。此外,在小鼠胆囊肝脏中,MABCA8B的蛋白质表达降低。胆汁淤积中MABCA8B表达水平的变化与MABCA1的MABCA1的变化相似,S正弦胆固醇流出转运蛋白。摄取和流出的测定结果表明,ABCA8介导[〜(3)H]胆固醇的流出和[〜(3)H] Taurocholate,同时它显示出[〜(3)H] Estrone硫酸盐的显着渗出活性,[〜(3 )H] Digoxin,[〜(3)H]压霉素,[〜(3)H]帕拉 - 氨基生物酸,[〜(3)H]油酸,[〜(14)c]尼古丁,或[〜(3 )H]甲氨蝶呤。 [〜(3)H]通过细胞外施用的牛磺酸盐增加胆固醇渗透。这些结果表明,MABCA8B / ABCA8用作小鼠和人肝中至少胆固醇和牛磺酸盐的胆固醇和牛磺酸盐的窦亢进输送器。

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