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MAL, an integral element of the apical sorting machinery, is an itinerant protein that cycles between the trans-Golgi network and the plasma membrane

机译:MAL是根尖分选机器的组成部分,是一种在高尔基反式网络和质膜之间循环的巡回蛋白

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摘要

The MAL proteolipid is a nonglycosylated integral membrane protein found in glycolipid-enriched membrane microdomains. In polarized epithelial Madin-Darby canine kidney cells, MAL is necessary for normal apical transport and accurate sorting of the influenza virus hemagglutinin. MAL is thus part of the integral machinery for glycolipid-enriched membrane-mediated apical transport. At steady state, MAL is predominantly located in perinuclear vesicles that probably arise from the trans-Golgi network (TGN). To act on membrane traffic and to prevent their accumulation in the target compartment, integral membrane elements of the protein-sorting machinery should be itinerant proteins that cycle between the donor and target compartments. To establish whether MAL is an itinerant protein, we engineered the last extracellular loop of MAL by insertion of sequences containing the FLAG epitope or with sequences containing residues that became O-glycosylated within the cells or that displayed biotinylatable groups. The ectopic expression of these modified MAL proteins allowed us to investigate the surface expression of MAL and its movement through different compartments after internalization with the use of a combination of assays, including surface biotinylation, surface binding of anti-FLAG antibodies, neuraminidase sensitivity, and drug treatments. Immunofluorescence and flow cytometric analyses indicated that, in addition to its Golgi localization, MAL was also expressed on the cell surface, from which it was rapidly internalized. This retrieval implies transport through the endosomal pathway and requires endosomal acidification, because it can be inhibited by drugs such as chloroquine, monensin, and NH4Cl. Resialylation experiments of surface MAL treated with neuraminidase indicated that ~30% of the internalized MAL molecules were delivered to the TGN, probably to start a new cycle of cargo transport. Together, these observations suggest that, as predicted for integral membrane members of the late protein transport machinery, MAL is an itinerant protein cycling between the TGN and the plasma membrane
机译:MAL蛋白脂是在富含糖脂的膜微区中发现的非糖基化的整合膜蛋白。在极化的上皮Madin-Darby犬肾细胞中,MAL对于正常的根尖运输和流感病毒血凝素的准确分选是必需的。因此,MAL是富含糖脂的膜介导的根尖运输的整体机制的一部分。在稳定状态下,MAL主要位于核周囊泡中,这可能是由反高尔基体网络(TGN)引起的。为了对膜运输起作用并防止其在靶区室中积聚,蛋白质分选机器的整体膜元件应为在供体区和靶区室之间循环的巡回蛋白。为了确定MAL是否是一种巡回蛋白,我们通过插入含有FLAG表位的序列或含有在细胞内被O-糖基化或显示出可生物素化基团的残基的序列,设计了MAL的最后一个细胞外环。这些修饰的MAL蛋白的异位表达使我们能够通过组合使用多种方法进行内部化研究,从而研究MAL的表面表达及其在不同区室中的移动,包括表面生物素化,抗FLAG抗体的表面结合,神经氨酸酶敏感性和药物治疗。免疫荧光和流式细胞仪分析表明,除高尔基体定位外,MAL还在细胞表面表达,并从中迅速内化。这种回收意味着通过内体途径运输,并且需要内体酸化,因为它可以被诸如氯喹,莫能菌素和NH4Cl之类的药物抑制。用神经氨酸酶处理的表面MAL的再唾液酸化实验表明,约30%的内在MAL分子被递送至TGN,可能开始了新的货物运输周期。总之,这些观察结果表明,正如晚期蛋白质转运机制中不可或缺的膜成员所预测的,MAL是TGN与质膜之间的一种巡回蛋白质循环

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