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Different ubiquitin signals act at the Golgi and plasma membrane to direct GAP1 trafficking

机译:不同的泛素信号作用于高尔基体和质膜,指导GAP1转运

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摘要

The high capacity general amino acid permease, Gap1p, in Saccharomyces cerevisiae is distributed between the plasma membrane and internal compartments according to availability of amino acids. When internal amino acid levels are low, Gap1p is localized to the plasma membrane where it imports available amino acids from the medium. When sufficient amino acids are imported, Gap1p at the plasma membrane is endocytosed and newly synthesized Gap1p is delivered to the vacuole; both sorting steps require Gap1p ubiquitination. Although it has been suggested that identical trans-acting factors and Gap1p ubiquitin acceptor sites are involved in both processes, we define unique requirements for each of the ubiquitin-mediated sorting steps involved in delivery of Gap1p to the vacuole upon amino acid addition. Our finding that distinct ubiquitin-mediated sorting steps employ unique trans-acting factors, ubiquitination sites on Gap1p, and types of ubiquitination demonstrates a previously unrecognized level of specificity in ubiquitin- mediated protein sorting.
机译:酿酒酵母中的高容量通用氨基酸通透酶Gap1p根据氨基酸的可用性分布在质膜和内部隔室之间。当内部氨基酸水平低时,Gap1p定位于质膜,从中导入可用的氨基酸。当输入足够的氨基酸时,质膜上的Gap1p被内吞,新合成的Gap1p被输送至液泡。这两个排序步骤都需要Gap1p泛素化。尽管已经建议在两个过程中都涉及相同的反式作用因子和Gap1p泛素受体位点,但我们为参与添加氨基酸后将Gap1p传递至液泡的泛素介导的分选步骤定义了独特的要求。我们的发现表明,独特的泛素介导的分选步骤利用独特的反式作用因子,Gap1p上的泛素化位点和泛素化的类型证明了在泛素介导的蛋白分选中先前无法识别的特异性水平。

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