Ma J, Lindquist S
Howard Hughes Medical Institute, Department of Molecular Genetics and Cell Biology, University of Chicago, 5841 S. Maryland Avenue MC1028, Chicago, Illinois 60637, USA.
Nat Cell Biol. 1999 Oct;1(6):358-61. doi: 10.1038/14053.
Conformational conversion of the cellular PrPC protein to PrPSc is a central aspect of the prion diseases, but how PrP initially converts to this conformation remains a mystery. Here we show that PrP expressed in the yeast cytoplasm, instead of the endoplasmic reticulum, acquires the characteristics of PrPSc, namely detergent insolubility and a distinct pattern of protease resistance. Neuroblastoma cells cultured under reducing, glycosylation-inhibiting conditions produce PrP with the same characteristics. We therefore describe what is, to our knowledge, the first conversion of full-length PrP in a heterologous system, show the importance of reducing and deglycosylation conditions in PrP conformational transitions, and suggest a model for initiating events in sporadic and inherited prion diseases.
细胞朊蛋白(PrPC)向瘙痒病相关纤维蛋白(PrPSc)的构象转变是朊病毒疾病的核心环节,但PrP最初如何转变为这种构象仍是个谜。在此我们表明,在酵母细胞质而非内质网中表达的PrP获得了PrPSc的特性,即去污剂不溶性和独特的蛋白酶抗性模式。在还原性、糖基化抑制条件下培养的神经母细胞瘤细胞产生具有相同特性的PrP。因此,据我们所知,我们描述了全长PrP在异源系统中的首次转变,展示了还原性和去糖基化条件在PrP构象转变中的重要性,并提出了一个散发性和遗传性朊病毒疾病起始事件的模型。
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