首页> 外文期刊>Genetics: A Periodical Record of Investigations Bearing on Heredity and Variation >Role of the Unfolded Protein Response Pathway in Secretory Stress and Regulation of INO1 Expression in Saccharomyces cerevisiae
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Role of the Unfolded Protein Response Pathway in Secretory Stress and Regulation of INO1 Expression in Saccharomyces cerevisiae

机译:展开的蛋白反应途径在酿酒酵母中分泌应激和INO1表达调控中的作用。

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The unfolded protein response pathway (UPR) enables the cell to cope with the buildup of unfolded proteins in the endoplasmic reticulum (ER). UPR loss-of-function mutants, hac1 Δ and ire1 Δ, are also inositol auxotrophs, a phenotype associated with defects in expression of INO1 , the most highly regulated of a set of genes encoding enzymes of phospholipid metabolism. We now demonstrate that the UPR plays a functional role in membrane trafficking under conditions of secretory stress in yeast. Mutations conferring a wide range of membrane trafficking defects exhibited negative genetic interaction when combined with ire1 Δ and hac1 Δ. At semipermissive temperatures, carboxypeptidase Y transit time to the vacuole was slower in Sec? cells containing an ire1 Δ or hac1 Δ mutation than in Sec? cells with an intact UPR. The UPR was induced in Sec? cells defective in subcellular membrane trafficking events ranging from ER vesicle trafficking to distal secretion and in erg6 Δ cells challenged with brefeldin A. However, the high levels of UPR induction observed under these conditions were not correlated with elevated INO1 expression. Indeed, many of the Sec? mutants that had elevated UPR expression at semipermissive growth temperatures failed to achieve wild-type levels of INO1 expression under these same conditions.
机译:未折叠的蛋白质反应途径(UPR)使细胞能够应付内质网(ER)中未折叠的蛋白质的积累。 UPR功能丧失的突变体hac1Δ和ire1Δ也是肌醇营养缺陷型,一种与INO1表达缺陷相关的表型,INO1是编码磷脂代谢酶的一组基因中调控最高的一组。现在我们证明,UPR在酵母中分泌应激的条件下在膜运输中发挥功能作用。当与ire1Δ和hac1Δ组合时,赋予多种膜运输缺陷的突变表现出负的遗传相互作用。在半容许温度下,Sec?中羧肽酶Y向液泡的传递时间较慢。含有ire1Δ或hac1Δ突变的细胞比Sec?具有完整UPR的细胞。普遍定期审议是在Sec?在从ER小泡运输到远端分泌的亚细胞膜运输事件中存在缺陷的细胞,以及在用布雷菲德菌素A攻击的erg6Δ细胞中存在缺陷。但是,在这些条件下观察到的高水平的UPR诱导与INO1表达升高无关。确实,许多秒?在相同的条件下,在半容许生长温度下具有UPR表达升高的突变体未能达到INO1表达的野生型水平。

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