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Monotopic topology is required for lipid droplet targeting of ancient ubiquitous protein 1

机译:单脂类拓扑学是脂质液滴靶向古代泛在蛋白1所必需的

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摘要

Ancient ubiquitous protein 1 (AUP1) is a multifunctional protein, which acts on both lipid droplets (LDs) and the endoplasmic reticulum (ER) membrane. Double localization to these two organelles, featuring very different membrane characteristics, was observed also for several other integral proteins, but little is known about the signals and mechanisms behind dual protein targeting to ER and LDs. Here we dissect the AUP1 targeting signals by analyses of localization and topology of several deletion and point mutants. We found that AUP1 is inserted into the membrane of the ER in a monotopic hairpin fashion, and subsequently transported to the hemi-membrane of LDs. A single domain localized in the N-terminal part of AUP1 enables its ER residence, the monotopic insertion, and the LD localization. Different specific residues within this multifunctional domain are responsible for achieving the complex spatial distribution pattern. A mutation of three amino acids, which changes AUP1 topology from hairpin to transmembrane, abolishes LD localization. These findings suggest that the cell is able to target a protein to multiple intracellular locations using a single domain.
机译:古代普遍存在的蛋白1(AUP1)是一种多功能蛋白,既作用于脂质滴(LDs),又作用于内质网(ER)膜。对于其他几种整合蛋白,还观察到了这两个细胞器的双重定位,它们具有非常不同的膜特性,但是对靶向ER和LD的双重蛋白背后的信号和机制知之甚少。在这里,我们通过分析几个缺失和点突变体的定位和拓扑来剖析AUP1靶向信号。我们发现,AUP1以单位发夹的方式插入ER的膜中,然后转运至LDs的半膜。定位在AUP1 N端部分的单个域可实现其ER驻留,单碱基插入和LD定位。该多功能域内的不同特定残基负责实现复杂的空间分布模式。三个氨基酸的突变将AUP1的拓扑结构从发夹变为跨膜,从而消除了LD的定位。这些发现表明,该细胞能够使用单个结构域将蛋白质靶向多个细胞内位置。

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