首页> 美国卫生研究院文献>Cell Regulation >Intracellular Trafficking of Bile Salt Export Pump (ABCB11) in Polarized Hepatic Cells: Constitutive Cycling between the Canalicular Membrane and rab11-positive Endosomes
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Intracellular Trafficking of Bile Salt Export Pump (ABCB11) in Polarized Hepatic Cells: Constitutive Cycling between the Canalicular Membrane and rab11-positive Endosomes

机译:胆汁盐输出泵(ABCB11)在极化的肝细胞内的细胞内贩运:小管膜和rab11阳性内体之间的本构循环。

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摘要

The bile salt export pump (BSEP, ABCB11) couples ATP hydrolysis with transport of bile acids into the bile canaliculus of hepatocytes. Its localization in the apical canalicular membrane is physiologically regulated by the demand to secrete biliary components. To gain insight into how such localization is regulated, we studied the intracellular trafficking of BSEP tagged with yellow fluorescent protein (YFP) in polarized WIF-B9 cells. Confocal imaging revealed that BSEP-YFP was localized at the canalicular membrane and in tubulo-vesicular structures either adjacent to the microtubule-organizing center or widely distributed in the cytoplasm. In the latter two locations, BSEP-YFP colocalized with rab11, an endosomal marker. Selective photobleaching experiments revealed that single BSEP-YFP molecules resided in canalicular membranes only transiently before exchanging with intracellular BSEP-YFP pools. Such exchange was inhibited by microtubule and actin inhibitors and was unaffected by brefeldin A, dibutyryl cyclic AMP, taurocholate, or PI 3-kinase inhibitors. Intracellular carriers enriched in BSEP-YFP elongated and dissociated as tubular elements from a globular structure adjacent to the microtubule-organizing center. They displayed oscillatory movement toward either canalicular or basolateral membranes, but only fused with the canalicular membrane. The pathway between canalicular and intracellular membranes that BSEP constitutively cycles within could serve to regulate apical pools of BSEP as well as other apical membrane transporters.
机译:胆汁盐输出泵(BSEP,ABCB11)将ATP水解与胆汁酸的运输耦合到肝细胞的胆小管中。其在根尖小管膜中的定位在生理上受到分泌胆汁成分的需求的调节。为了深入了解如何调节这种定位,我们研究了极化WIF-B9细胞中标记有黄色荧光蛋白(YFP)的BSEP的细胞内运输。共聚焦成像显示BSEP-YFP位于小管膜和微管组织中心附近或广泛分布于细胞质的微管结构中。在后两个位置,BSEP-YFP与内体标记rab11共定位。选择性光漂白实验表明,单个BSEP-YFP分子仅在与细胞内BSEP-YFP池交换之前短暂驻留在小管膜中。这种交换受到微管和肌动蛋白抑制剂的抑制,而不受布雷菲德菌素A,二丁酰环AMP,牛磺胆酸盐或PI 3-激酶抑制剂的影响。富含BSEP-YFP的细胞内载体从与微管组织中心相邻的球状结构中伸长并解离为管状元素。它们显示出朝向小管或基底外侧膜的振荡运动,但仅与小管膜融合。 BSEP组成性循环的小管膜和细胞内膜之间的通路可用于调节BSEP的顶池以及其他顶膜转运蛋白。

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