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Requirement for Neo1p in retrograde transport from the Golgi complex to the endoplasmic reticulum

机译:从高尔基体到内质网逆向转运Neo1p的要求

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Neo1p from Saccharomyces cerevisiae is an essential P-type ATPase and potential aminophospholipid translocase (flippase) in the Drs2p family. We have previously implicated Drs2p in protein transport steps in the late secretory pathway requiring ADP-ribosylation factor (ARE) and clathrin. Here, we present evidence that epitope-tagged Neo1p localizes to the endoplasmic reticulum (ER) and Golgi complex and is required for a retrograde transport pathway between these organelles. Using conditional alleles of NEO1, we find that loss of Neo1p function causes cargo-specific defects in anterograde protein transport early in the secretory pathway and perturbs glycosylation in the Golgi complex. Rer1-GFP, a protein that cycles between the ER and Golgi complex in COPI and COPII vesicles, is mislocalized to the vacuole in neo1-ts at the nonpermissive temperature. These phenotypes suggest that the anterograde protein transport defect is a secondary consequence of a defect in a COPI-dependent retrograde pathway. We propose that loss of lipid asymmetry in the cis Golgi perturbs retrograde protein transport to the ER. [References: 50]
机译:酿酒酵母中的Neo1p是Drs2p家族中必不可少的P型ATPase和潜在的氨基磷脂转位酶(flippase)。我们以前牵涉到Drs2p参与需要ADP-核糖基化因子(ARE)和网格蛋白的晚期分泌途径中的蛋白质运输步骤。在这里,我们提供证据,标记抗原决定簇的Neo1p定位于内质网(ER)和高尔基体,并且是这些细胞器之间逆行运输途径所必需的。使用NEO1的条件等位基因,我们发现Neo1p功能的丧失会在分泌途径的早期导致顺行蛋白质运输中的货物特异性缺陷,并扰乱高尔基体中的糖基化。 Rer1-GFP是一种在COP1和COPII囊泡中的ER和高尔基复合体之间循环的蛋白质,在非允许温度下在neo1-ts中被错误定位在液泡中。这些表型表明顺行蛋白质转运缺陷是COPI依赖性逆行途径缺陷的次要结果。我们提出,在顺式高尔基体中脂质不对称性的损失扰乱了向ER的逆行蛋白转运。 [参考:50]

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