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内侧高尔基体离子泵Pmr1为酵母分泌途径提供糖基化、分选和内质网相关蛋白降解所需的Ca2+和Mn2+。

The medial-Golgi ion pump Pmr1 supplies the yeast secretory pathway with Ca2+ and Mn2+ required for glycosylation, sorting, and endoplasmic reticulum-associated protein degradation.

作者信息

Dürr G, Strayle J, Plemper R, Elbs S, Klee S K, Catty P, Wolf D H, Rudolph H K

机构信息

Institut für Biochemie der Universität Stuttgart, D-70569 Stuttgart, Germany.

出版信息

Mol Biol Cell. 1998 May;9(5):1149-62. doi: 10.1091/mbc.9.5.1149.

Abstract

The yeast Ca2+ adenosine triphosphatase Pmr1, located in medial-Golgi, has been implicated in intracellular transport of Ca2+ and Mn2+ ions. We show here that addition of Mn2+ greatly alleviates defects of pmr1 mutants in N-linked and O-linked protein glycosylation. In contrast, accurate sorting of carboxypeptidase Y (CpY) to the vacuole requires a sufficient supply of intralumenal Ca2+. Most remarkably, pmr1 mutants are also unable to degrade CpY*, a misfolded soluble endoplasmic reticulum protein, and display phenotypes similar to mutants defective in the stress response to malfolded endoplasmic reticulum proteins. Growth inhibition of pmr1 mutants on Ca2+-deficient media is overcome by expression of other Ca2+ pumps, including a SERCA-type Ca2+ adenosine triphosphatase from rabbit, or by Vps10, a sorting receptor guiding non-native luminal proteins to the vacuole. Our analysis corroborates the dual function of Pmr1 in Ca2+ and Mn2+ transport and establishes a novel role of this secretory pathway pump in endoplasmic reticulum-associated processes.

摘要

位于高尔基体中部的酵母钙离子三磷酸腺苷酶Pmr1与钙离子和锰离子的细胞内运输有关。我们在此表明,添加锰离子可极大地缓解pmr1突变体在N-连接和O-连接蛋白糖基化方面的缺陷。相比之下,将羧肽酶Y(CpY)准确分选至液泡需要腔内有足够的钙离子供应。最显著的是,pmr1突变体也无法降解CpY*(一种错误折叠的可溶性内质网蛋白),并表现出与内质网错误折叠蛋白应激反应缺陷突变体相似的表型。在缺钙培养基上,pmr1突变体的生长抑制可通过表达其他钙离子泵(包括来自兔子的一种肌浆网钙离子三磷酸腺苷酶)或Vps10(一种将非天然腔内蛋白导向液泡的分选受体)来克服。我们的分析证实了Pmr1在钙离子和锰离子运输中的双重功能,并确立了这种分泌途径泵在内质网相关过程中的新作用。

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