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含细胞朊蛋白及其瘙痒病异构体的去污剂不溶性复合物的特性分析。

Characterization of detergent-insoluble complexes containing the cellular prion protein and its scrapie isoform.

作者信息

Naslavsky N, Stein R, Yanai A, Friedlander G, Taraboulos A

机构信息

Department of Molecular Biology, the Hebrew University-Hadassah Medical School, P. O. Box 12272, Jerusalem 91120, Israel.

出版信息

J Biol Chem. 1997 Mar 7;272(10):6324-31. doi: 10.1074/jbc.272.10.6324.

Abstract

Cells infected with prions contain both prion protein isoforms cellular prion protein (PrPC) and scrapie prion protein (PrPSc). PrPSc is formed posttranslationally through the pathological refolding of PrPC. In scrapie-infected ScN2a cells, the metabolism of both PrP isoforms involves cholesterol-dependent pathways. We show here that both PrPC and PrPSc are attached to Triton X-100-insoluble, low-density complexes or "rafts." These complexes are sensitive to saponin and thus probably contain cholesterol. This finding suggests that the transformation PrPC --> PrPSc occurs within rafts. It also reveals the existence of rafts in late compartments of the endocytic pathway, where most PrPSc resides. When Triton X-100 lysates of cells were incubated at 37 degrees C prior to density analysis, PrPC was still found in buoyant complexes, although it now failed to sediment at high speed. This property was shared by another glycophosphatidyl inositol protein, Thy-1, and also by the raft resident GM1. In one ScN2a clone and in the brain of a Syrian hamster with scrapie, Triton X-100 extraction at 37 degrees C permitted resolution of PrPC and PrPSc into two distinct peaks of different densities. This suggests that there are two populations of PrP-containing rafts and may permit isolation of PrPC-specific rafts from those containing PrPSc. Our findings reinforce the contention that rafts are involved in various aspects of PrP metabolism and in the "life cycle" of prions.

摘要

感染朊病毒的细胞同时含有两种朊病毒蛋白异构体,即细胞朊病毒蛋白(PrPC)和瘙痒病朊病毒蛋白(PrPSc)。PrPSc是通过PrPC的病理性重折叠在翻译后形成的。在感染瘙痒病的ScN2a细胞中,两种PrP异构体的代谢都涉及胆固醇依赖性途径。我们在此表明,PrPC和PrPSc都附着于Triton X-100不溶性低密度复合物或“脂筏”上。这些复合物对皂素敏感,因此可能含有胆固醇。这一发现表明PrPC向PrPSc的转变发生在脂筏内。它还揭示了内吞途径晚期区室中脂筏的存在,大多数PrPSc存在于该区室。当细胞的Triton X-100裂解物在密度分析前于37℃孵育时,仍可在漂浮复合物中发现PrPC,尽管此时它已无法高速沉淀。另一种糖基磷脂酰肌醇蛋白Thy-1以及脂筏驻留分子GM1也具有这一特性。在一个ScN2a克隆和一只患有瘙痒病的叙利亚仓鼠的大脑中,37℃下用Triton X-100提取可将PrPC和PrPSc分离为两个不同密度的峰。这表明存在两种含PrP的脂筏群体,并且可能允许从含有PrPSc的脂筏中分离出PrPC特异性脂筏。我们的发现强化了脂筏参与PrP代谢的各个方面以及朊病毒“生命周期”的观点。

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