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通过用还原剂处理细胞,使分泌蛋白选择性保留在酵母内质网中。

Selective retention of secretory proteins in the yeast endoplasmic reticulum by treatment of cells with a reducing agent.

作者信息

Jämsä E, Simonen M, Makarow M

机构信息

Institute of Biotechnology, University of Helsinki, Finland.

出版信息

Yeast. 1994 Mar;10(3):355-70. doi: 10.1002/yea.320100308.

DOI:10.1002/yea.320100308
PMID:8017105
Abstract

We have used four glycoproteins as markers to study how disulfide bond formation and protein folding effect the intracellular transport of proteins in yeast. Under normal conditions, the vacuolar enzyme carboxypeptidase Y (CPY) and the secretory stress-protein hsp150 acquired disulfide bonds in the endoplasmic reticulum (ER). Treatment of living cells with the reducing agent dithiothreitol (DTT) prevented disulfide formation of newly synthesized CPY and hsp150, resulting in retention of the proteins in the ER. When DTT was removed, the sulfhydryls were reoxidized, and the transport of the proteins to their correct destinations was resumed. Even mature CPY, located in the vacuole, could be reduced with DTT, and reoxidized after removal of the drug. DTT treatment blocked intracellular transport of hsp150 only when present during the synthesis and translocation of the protein. Reduction of folded hsp150, accumulated in the ER due to a sec block prior to DTT treatment, did not inhibit its secretion. The Kar2p/BiP protein, a component of the ER lumen, was found to be associated with fully translocated reduced hsp150, but not with native hsp150, suggesting that Kar2p/BiP may be involved in the putative retention mechanism. The cysteine-free pro-alpha-factor, and invertase which was shown to have free sulfhydryls, were secreted and modified similarly in the presence and absence of DTT, showing that the secretory pathway of yeast functioned under reducing conditions.

摘要

我们使用了四种糖蛋白作为标记物,来研究二硫键形成和蛋白质折叠如何影响酵母中蛋白质的细胞内运输。在正常情况下,液泡酶羧肽酶Y(CPY)和分泌应激蛋白hsp150在内质网(ER)中形成二硫键。用还原剂二硫苏糖醇(DTT)处理活细胞可阻止新合成的CPY和hsp150形成二硫键,导致这些蛋白质滞留在内质网中。当去除DTT后,巯基重新氧化,蛋白质恢复向其正确目的地的运输。即使位于液泡中的成熟CPY,也能用DTT还原,并在去除药物后重新氧化。只有在蛋白质合成和转运过程中存在DTT时,它才会阻断hsp150的细胞内运输。对由于DTT处理前的sec阻断而在内质网中积累的折叠hsp150进行还原,并不抑制其分泌。发现内质网腔成分Kar2p/BiP蛋白与完全转运的还原型hsp150相关,但与天然hsp150不相关,这表明Kar2p/BiP可能参与了假定的滞留机制。无半胱氨酸的前α因子和已证明具有游离巯基的蔗糖酶,在有和没有DTT的情况下分泌和修饰方式相似,这表明酵母的分泌途径在还原条件下起作用。

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