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转染的犬肾细胞(Madin-Darby canine kidney cells)中乙肝表面抗原的顶端分泌

Apical secretion of hepatitis B surface antigen from transfected Madin-Darby canine kidney cells.

作者信息

González A, Nicovani S, Juica F

机构信息

Departamento de Immunología Clínica y Reumatología, Facultad de Medicina, P. Universidad Católica de Chile, Santiago.

出版信息

J Biol Chem. 1993 Mar 25;268(9):6662-7.

PMID:8454638
Abstract

Hepatitis B surface antigen (HBsAg), the major envelope component of human hepatitis B virus, during infection drives the assembly and basolateral secretion from hepatocytes of both virions and subviral lipoprotein particles into the bloodstream. We studied the sorting behavior of HBsAg in the heterologous epithelial Madin-Darby canine kidney cells permanently transformed with the hepatitis B virus S gene. These cells, forming tightly packed monolayers in permeable supports, secreted HBsAg apically through a mechanism not involving transcytosis. This suggests that molecular features acting as apical addressing information, seemingly unfunctional or less efficiently used by the exocytic machinery of hepatocytes, could be contained in short hydrophilic regions of HBsAg. Lipids also could play a role in this asymmetric sorting because HBsAg is known to be secreted by forming macromolecular lipoprotein complexes rather than as a soluble protein. Together with available data, our results would imply not only the existence of tissue-specific variations in handling constitutively secreted proteins but also that these variations are strikingly dependent on the kind of protein examined. On the other hand, pulse-chase experiments with tunicamycin showed that the expression of apical information in HBsAg particles does not require N-linked glycosylation, contrasting with the known gp80 Madin-Darby canine kidney-endogenous apical secretory marker. This is the first experimental evidence that carbohydrate moieties in secretory proteins do not hold domain-specific sorting signals, a fact previously shown exclusively for membrane proteins. Thus, HBsAg provides a novel model system for the analysis of the molecular mechanisms of constitutive apical secretion.

摘要

乙肝表面抗原(HBsAg)是人类乙肝病毒主要的包膜成分,在感染过程中驱动病毒粒子和亚病毒脂蛋白颗粒从肝细胞组装并通过基底外侧分泌进入血液循环。我们研究了用乙肝病毒S基因永久转化的异源上皮性马-达二氏犬肾细胞中HBsAg的分选行为。这些细胞在可渗透支持物上形成紧密堆积的单层,通过一种不涉及转胞吞作用的机制将HBsAg分泌到顶端。这表明,作为顶端定位信息的分子特征可能包含在HBsAg的短亲水区中,而这些特征在肝细胞的胞吐机制中似乎不起作用或使用效率较低。脂质也可能在这种不对称分选中发挥作用,因为已知HBsAg是通过形成大分子脂蛋白复合物而不是作为可溶性蛋白分泌的。结合现有数据,我们的结果不仅意味着在处理组成型分泌蛋白时存在组织特异性差异,而且这些差异明显取决于所检测的蛋白种类。另一方面,用衣霉素进行的脉冲追踪实验表明,HBsAg颗粒中顶端信息的表达不需要N-糖基化,这与已知的马-达二氏犬肾内源性顶端分泌标记物gp80形成对比。这是第一个实验证据表明分泌蛋白中的碳水化合物部分不携带结构域特异性分选信号,这一事实此前仅在膜蛋白中得到证实。因此,HBsAg为分析组成型顶端分泌的分子机制提供了一个新的模型系统。

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Apical secretion of hepatitis B surface antigen from transfected Madin-Darby canine kidney cells.转染的犬肾细胞(Madin-Darby canine kidney cells)中乙肝表面抗原的顶端分泌
J Biol Chem. 1993 Mar 25;268(9):6662-7.
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Apical sorting of a voltage- and Ca2+-activated K+ channel alpha -subunit in Madin-Darby canine kidney cells is independent of N-glycosylation.在麦迪逊-达比犬肾细胞中,电压和钙离子激活的钾通道α亚基的顶端分选独立于N-糖基化。
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Intracellular transport and secretion of hepatitis B surface antigen in mammalian cells.乙型肝炎表面抗原在哺乳动物细胞内的转运与分泌
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MAL mediates apical transport of secretory proteins in polarized epithelial Madin-Darby canine kidney cells.MAL介导极化上皮性犬肾细胞中分泌蛋白的顶端运输。
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Cholesterol depletion reduces apical transport capacity in epithelial Madin-Darby canine kidney cells.胆固醇耗竭降低了上皮性犬肾细胞(Madin-Darby canine kidney cells)的顶端转运能力。
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