首页> 外文期刊>Journal of cell biology >Transport of influenza HA from the trans-Golgi network to the apical surface of MDCK cells permeabilized in their basolateral plasma membranes: energy dependence and involvement of GTP-binding proteins.
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Transport of influenza HA from the trans-Golgi network to the apical surface of MDCK cells permeabilized in their basolateral plasma membranes: energy dependence and involvement of GTP-binding proteins.

机译:流感HA从反高尔基体网络到其基底外侧质膜中透化的MDCK细胞的顶表面的运输:能量依赖性和GTP结合蛋白的参与。

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A procedure employing streptolysin O to effect the selective permeabilization of either the apical or basolateral plasma membrane domains of MDCK cell monolayers grown on a filter support was developed which permeabilizes the entire monolayer, leaves the opposite cell surface domain intact, and does not abolish the integrity of the tight junctions. This procedure renders the cell interior accessible to exogenous macromolecules and impermeant reagents, permitting the examination of their effects on membrane protein transport to the intact surface. The last stages of the transport of the influenza virus hemagglutinin (HA) to the apical surface were studied in pulse-labeled, virus-infected MDCK cells that were incubated at 19.5 degrees C for 90 min to accumulate newly synthesized HA in the trans-Golgi network (TGN), before raising the temperature to 35 degrees C to allow synchronized transport to the plasma membrane. In cells permeabilized immediately after the cold block, 50% of the intracellular HA molecules were subsequently delivered to the apical surface. This transport was dependent on the presence of an exogenous ATP supply and was markedly inhibited by the addition of GTP-gamma-S at the time of permeabilization. On the other hand, the GTP analogue had no effect when it was added to cells that, after the cold block, were incubated for 15 min at 35 degrees C before permeabilization, even though at this time most HA molecules were still intracellular and their appearance at the cell surface was largely dependent on exogenous ATP. These findings indicate that GTP-binding proteins are involved in the constitutive process that effects vesicular transport from the TGN to the plasma membrane and that they are charged early in this process. Transport of HA to the cell surface could be made dependent on the addition of exogenous cytosol when, after permeabilization, cells were washed to remove endogenous cytosolic components. This opens the way towards the identification of cell components that mediate the sorting of apical and basolateral membrane components in the TGN and their polarized delivery to the cell surface.
机译:开发了一种使用链球菌溶血素O来选择性过滤通透在滤膜支持物上的MDCK细胞单层的顶端或基底外侧质膜结构域的方法,该方法可透化整个单层膜,使相对的细胞表面结构域完整无损,并且不会破坏完整性的紧密连接。此过程使细胞内部易于接触外源大分子和不渗透试剂,从而可以检查它们对膜蛋白转运至完整表面的影响。在脉冲标记的病毒感染的MDCK细胞中研究了流感病毒血凝素(HA)向顶端表面运输的最后阶段,将其在19.5摄氏度下孵育90分钟,以在反式高尔基体中积累新合成的HA网络(TGN),然后将温度升高到35摄氏度,以允许同步传输到质膜。在冷阻滞后立即通透的细胞中,50%的细胞内HA分子随后被递送至顶端表面。这种转运取决于外源ATP供应的存在,并且在透化时显着被GTP-γ-S的添加所抑制。另一方面,将GTP类似物加入冷冷后在透化之前于35℃孵育15分钟的细胞中没有作用,即使此时大多数HA分子仍在细胞内并且其外观在细胞表面很大程度上依赖于外源性ATP。这些发现表明,GTP结合蛋白参与了影响囊泡从TGN转运到质膜的组成过程,并且在该过程的早期它们被带电。当透化后,洗涤细胞以去除内源性胞质成分时,可根据是否添加外源性细胞质来使HA转运至细胞表面。这为鉴定介导TGN中顶膜和基底外侧膜成分的分类及其极化递送至细胞表面的细胞成分开辟了道路。

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