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Ykt6p is a multifunctional yeast R-SNARE that is required for multiple membrane transport pathways to the vacuole

机译:Ykt6p是多功能酵母R-SNARE,它是到达膜泡的多种膜转运途径所必需的

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Intracellular membrane fusion requires that membrane-bound soluble N-ethylmaleimide-sensitive factor attachment protein receptor (SNARE) proteins on both vesicle and target membranes form a highly specific complex necessary to bring the membranes close in space. Ykt6p is a yeast R-SNARE protein that has been implicated in retrograde transport to the cis-Golgi compartment. Ykt6p has been also been found to fractionate with vacuole membranes and participate in a vacuolar SNARE complex in homotypic vacuole fusion. To investigate the role of Ykt6p in membrane traffic to the vacuole we generated temperature-sensitive mutations in YKT6. One mutation produces an early Golgi block to secretion, and overexpression of the SNARE protein Sft1p suppresses the growth and secretion defects of this mutation. These results are consistent with Ykt6p and Sft1p participating in a SNARE complex associated with retrograde transport to the cis-Golgi. A second set of mutations in YKT6 specifically affects post-Golgi membrane traffic to the vacuole, and the effects of these mutations are not suppressed by Sft1p overexpression. Defects are seen in carboxypeptidase Y sorting, alkaline phosphatase transport, and aminopeptidase I delivery, and in one mutant, overexpression of the SNARE protein Nyv1p suppresses the alkaline phosphatase transport defect. By mutationally separating early and late requirements for Ykt6p, our findings have revealed that Ykt6p is a R-SNARE protein that functions directly in the three biosynthetic pathways to the vacuole. [References: 61]
机译:细胞内膜融合需要囊泡和靶膜上的膜结合的可溶性N-乙基马来酰亚胺敏感因子附着蛋白受体(SNARE)蛋白形成高度特异性的复合物,以使膜在空间上紧密结合。 Ykt6p是一种酵母R-SNARE蛋白,与逆向运输至顺式高尔基体有关。还发现Ykt6p与液泡膜分离并参与同型液泡融合中的液泡SNARE复合物。为了研究Ykt6p在膜运输至液泡中的作用,我们在YKT6中产生了温度敏感性突变。一个突变产生早期的高尔基体分泌阻滞,而SNARE蛋白Sft1p的过表达抑制了该突变的生长和分泌缺陷。这些结果与Ykt6p和Sft1p参与与逆向转运至顺式高尔基体相关的SNARE复合体有关。 YKT6中的第二组突变特别影响高尔基体后液泡到达液泡,Sft1p过表达不会抑制这些突变的影响。在羧肽酶Y分选,碱性磷酸酶转运和氨基肽酶I转运中发现缺陷,并且在一个突变体中,SNARE蛋白Nyv1p的过表达抑制了碱性磷酸酶转运缺陷。通过突变分离对Ykt6p的早期和晚期需求,我们的发现表明Ykt6p是一种R-SNARE蛋白,直接在通往液泡的三种生物合成途径中起作用。 [参考:61]

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