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鉴定和表征对哺乳动物朊病毒有效的药物的方法:从基于酵母的抗朊病毒药物筛选试验到体内小鼠模型

Procedure for identification and characterization of drugs efficient against mammalian prion: from a yeast-based antiprion drug screening assay to in vivo mouse models.

作者信息

Voisset Cécile, Saupe Sven J, Galons Hervé, Blondel Marc

机构信息

INSERM U613, Brest, F-29200, France.

出版信息

Infect Disord Drug Targets. 2009 Feb;9(1):31-9. doi: 10.2174/1871526510909010031.

DOI:10.2174/1871526510909010031
PMID:19200013
Abstract

Prion diseases are fatal and incurable infectious neurodegenerative disorders affecting humans and other mammals. Prions are composed essentially if not solely of PrP(Sc), a misfolded form of the host-encoded PrP protein. PrP(Sc) catalyzes the transconformation of the normal endogenous PrP (PrP(C)) into more PrP(Sc). Prion replication thus corresponds to the propagation of an altered folding state of PrP. Several prion proteins have also been identified in the simple model organism Saccharomyces cerevisiae. Yeast prion-based screening assays have allowed identification of drugs active against mammalian prions, thus revealing the existence of common prion propagation mechanisms conserved from yeast to human. To identify these conserved targets, antiprion compounds isolated in yeast can be used as baits in reverse screening strategies. Once identified, these targets could in turn lead to the development of mechanism-based cell-free antiprion screening assays. A reverse screening procedure has been performed for 6AP and GA, two antiprion compounds isolated using a yeast-based assay. Protein folding activity of the large ribosomal RNA was found to be a physical and a functional target of both 6AP and GA therefore suggesting that this activity of the ribosome may constitute a novel mechanism involved in prion propagation and, as a consequence, a new screening target.

摘要

朊病毒疾病是一种致命且无法治愈的传染性神经退行性疾病,影响人类和其他哺乳动物。朊病毒本质上(如果不是仅仅)由PrP(Sc)组成,它是宿主编码的PrP蛋白的错误折叠形式。PrP(Sc)催化正常内源性PrP(PrP(C))转变为更多的PrP(Sc)。因此,朊病毒复制对应于PrP改变的折叠状态的传播。在简单的模式生物酿酒酵母中也发现了几种朊病毒蛋白。基于酵母朊病毒的筛选试验已经能够鉴定出对哺乳动物朊病毒有活性的药物,从而揭示了从酵母到人类保守的常见朊病毒传播机制的存在。为了鉴定这些保守的靶点,在酵母中分离出的抗朊病毒化合物可以用作反向筛选策略中的诱饵。一旦确定,这些靶点反过来可能会导致基于机制的无细胞抗朊病毒筛选试验的开发。已经对6AP和GA进行了反向筛选程序,这两种抗朊病毒化合物是使用基于酵母的试验分离出来的。发现大核糖体RNA的蛋白质折叠活性是6AP和GA的物理和功能靶点,因此表明核糖体的这种活性可能构成参与朊病毒传播的一种新机制,因此是一个新的筛选靶点。

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Protein Folding Activity of the Ribosome is involved in Yeast Prion Propagation.核糖体的蛋白质折叠活性参与酵母朊病毒的传播。
Sci Rep. 2016 Sep 16;6:32117. doi: 10.1038/srep32117.
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