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酵母质膜上的多药转运蛋白Pdr5在内吞作用之前被泛素化,并在液泡中降解。

The yeast multidrug transporter Pdr5 of the plasma membrane is ubiquitinated prior to endocytosis and degradation in the vacuole.

作者信息

Egner R, Kuchler K

机构信息

Department of Molecular Genetics, University and Biocenter Vienna, Austria.

出版信息

FEBS Lett. 1996 Jan 8;378(2):177-81. doi: 10.1016/0014-5793(95)01450-0.

Abstract

We have recently demonstrated that the Pdr5 ATP binding cassette multidrug transporter is a short-lived protein, whose biogenesis involves cell surface targeting followed by endocytosis and delivery to the vacuole for proteolytic turnover [Egner, R., Mahé, Y., Pandjaitan, R., and Kuchler, K. (1995) Mol. Cell. Biol. 15, 5879-5887]. Using c-myc epitope-tagged ubiquitin, we now have shown that Pdr5 is a ubiquitinated plasma membrane protein in vivo. Ubiquitination of Pdr5 was detected in both wild type and conditional end mutants defective in endocytic vesicle formation. Likewise, the Ste6 a-factor pheromone transporter, which represents another short-lived ABC transporter whose turnover requires vacuolar proteolysis, was also found to be ubiquitinated, and ubiquitin-modified Ste6 massively accumulated in end4 mutants at the restrictive temperature. By contrast, the plasma membrane ATPase Pma1, a long-lived and metabolically very stable protein, was found not to be ubiquitinated. Our results imply a novel function for ubiquitin in protein trafficking and suggest that ubiquitination of certain short-lived plasma membrane proteins may trigger their endocytic delivery to the vacuole for proteolytic turnover.

摘要

我们最近证实,Pdr5 ATP结合盒多药转运蛋白是一种寿命较短的蛋白质,其生物合成过程包括靶向细胞表面,随后通过内吞作用转运至液泡进行蛋白水解更新[Egner, R., Mahé, Y., Pandjaitan, R., and Kuchler, K. (1995) Mol. Cell. Biol. 15, 5879 - 5887]。利用c-myc表位标签标记的泛素,我们现已证明Pdr5在体内是一种泛素化的质膜蛋白。在野生型和内吞小泡形成缺陷的条件性内吞突变体中均检测到Pdr5的泛素化。同样,Ste6 a因子信息素转运蛋白,它是另一种寿命较短的ABC转运蛋白,其更新需要液泡蛋白水解作用,也被发现是泛素化的,并且在限制温度下,泛素修饰的Ste6在end4突变体中大量积累。相比之下,质膜ATP酶Pma1是一种寿命较长且代谢非常稳定的蛋白质,未发现其被泛素化。我们的结果暗示了泛素在蛋白质转运中的新功能,并表明某些寿命较短的质膜蛋白的泛素化可能会触发它们通过内吞作用转运至液泡进行蛋白水解更新。

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