朊病毒蛋白肽(PrP106-126)的细胞毒性与阿尔茨海默病淀粉样肽Aβ25-35的细胞毒性作用机制不同

James Hope , Mark S. Shearman , Helen C. Baxter , Angela Chong , Sharon M. Kelly , Nicholas C. Price
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引用次数: 67

摘要

朊病毒蛋白(PrPSc)的异常形式,一种合成的朊病毒蛋白肽片段(PrP106-126)和阿尔茨海默氏症蛋白前体APP的片段,已被证明在体外具有细胞毒性。我们使用了最初用于研究阿尔茨海默病淀粉样蛋白肽Aβ25-35毒性的同步克隆细胞模型来研究PrP肽的作用。我们发现,PrP106–126的细胞毒性取决于其聚集状态和PrPC的细胞表达,并且在没有与aβ25–35的细胞效应相关的细胞死亡的情况下,与MTT还原活性的丧失无关。这些因素可能在朊病毒蛋白相关疾病的不同病理表型的病变特异性中发挥作用。
本文章由计算机程序翻译,如有差异,请以英文原文为准。
Cytotoxicity of Prion Protein Peptide (PrP106–126) Differs in Mechanism from the Cytotoxic Activity of the Alzheimer's Disease Amyloid Peptide, Aβ25–35

The abnormal form of the prion protein (PrPSc), a synthetic prion protein peptide fragment (PrP106–126) and fragments of the Alzheimer's protein precursor, APP, have been shown to be cytotoxicin vitro.We have used synchronous, clonal cell models originally developed to study the toxicity of the Alzheimer's disease amyloid peptide, Aβ25–35, to investigate the actions of PrP peptides. We found that the cytotoxicity of the PrP106–126depends on its state of aggregation and the cellular expression of PrPC, and is independent of a loss of MTT reduction activity in the absence of cell death associated with the cellular effects of Aβ25–35. These factors may play a role in the lesion specificity of different pathological phenotypes of prion-protein related diseases.

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