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磷脂酰胆碱在极化HepG2细胞中的囊泡运输和非囊泡运输

Vesicular and nonvesicular transport of phosphatidylcholine in polarized HepG2 cells.

作者信息

Wüstner D, Mukherjee S, Maxfield F R, Müller P, Herrmann A

机构信息

Humboldt-Universität zu Berlin, Mathematisch-Naturwissenschaftliche Fakultät I, Institut für Biologie/Biophysik, Invalidenstr. 43, D-10115 Berlin, Germany.

出版信息

Traffic. 2001 Apr;2(4):277-96. doi: 10.1034/j.1600-0854.2001.9o135.x.

Abstract

We have investigated the transport and canalicular enrichment of fluorescent phosphatidylcholine (PC) in HepG2 cells using the fluorescent analogs of PC C6-NBD-PC and beta-BODIPY-PC. Fluorescent PC was efficiently transported to the biliary canaliculus (BC) and became enriched on the lumenal side of the canalicular membrane as shown for C6-NBD-PC. Some fluorescent PC was transported in vesicles to a subapical compartment (SAC) or apical recycling compartment (ARC) in polarized HepG2 cells as shown by colocalization with fluorescent sphingomyelin (C6-NBD-SM) and fluorescent transferrin, respectively. Extensive trafficking of vesicles containing fluorescent PC between the basolateral domain, the SAC/ARC and the BC as well as endocytosis of PC analogs from the canalicular membrane were found. Evidence for nonvesicular transport included enrichment of the PC-analog beta-BODIPY-PC in the BC (t1/2 = 3.54 min) prior to its accumulation in the SAC/ARC (t1/2 = 18.5 min) at 37 degrees C. Transport of fluorescent PC to the canalicular membrane also continued after disruption of the actin or microtubule cytoskeleton and at 2 degrees C. These results indicate that: (i) a nonvesicular transport pathway significantly contributes to the canalicular enrichment of PC in hepatocytic cells, and (ii) vesicular transport of fluorescent PC occurs from both membrane domains via the SAC/ARC.

摘要

我们使用磷脂酰胆碱(PC)的荧光类似物C6-NBD-PC和β-硼二吡咯-PC,研究了荧光PC在HepG2细胞中的转运和胆小管富集情况。如C6-NBD-PC所示,荧光PC被有效地转运至胆小管(BC),并在胆小管膜的管腔侧富集。一些荧光PC以囊泡形式分别与荧光鞘磷脂(C6-NBD-SM)和荧光转铁蛋白共定位,转运至极化HepG2细胞的顶下区室(SAC)或顶端回收区室(ARC)。发现含有荧光PC的囊泡在基底外侧结构域、SAC/ARC和BC之间广泛运输,以及PC类似物从胆小管膜的内吞作用。非囊泡运输的证据包括在37℃时,PC类似物β-硼二吡咯-PC在BC中的富集(t1/2 = 3.54分钟)先于其在SAC/ARC中的积累(t1/2 = 18.5分钟)。在肌动蛋白或微管细胞骨架破坏后以及在2℃时,荧光PC向胆小管膜的转运仍在继续。这些结果表明:(i)非囊泡运输途径对肝细胞中PC的胆小管富集有显著贡献,(ii)荧光PC的囊泡运输通过SAC/ARC从两个膜结构域发生。

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