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首页> 外文期刊>Molecular Neurobiology >A Single Amino Acid Substitution, Found in Mammals with Low Susceptibility to Prion Diseases, Delays Propagation of Two Prion Strains in Highly Susceptible Transgenic Mouse Models
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A Single Amino Acid Substitution, Found in Mammals with Low Susceptibility to Prion Diseases, Delays Propagation of Two Prion Strains in Highly Susceptible Transgenic Mouse Models

机译:在对朊病毒疾病的敏感性低的哺乳动物中发现单一的氨基酸取代,在高易感转基因小鼠模型中延迟了两种朊病毒菌株的繁殖

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Specific variations in the amino acid sequence of prion protein (PrP) are key determinants of susceptibility to prion diseases. We previously showed that an amino acid substitution specific to canids confers resistance to prion diseases when expressed in mice and demonstrated its dominant-negative protective effect against a variety of infectious prion strains of different origins and characteristics. Here, we show that expression of this single amino acid change significantly increases survival time in transgenic mice expressing bank vole cellular prion protein (PrP (c)), which is inherently prone to misfolding, following inoculation with two distinct prion strains (the CWD-vole strain and an atypical strain of spontaneous origin). This amino acid substitution hinders the propagation of both prion strains, even when expressed in the context of a PrP (c) uniquely susceptible to a wide range of prion isolates. Non-inoculated mice expressing this substitution experience spontaneous prion formation, but showing an increase in survival time comparable to that observed in mutant mice inoculated with the atypical strain. Our results underscore the importance of this PrP variant in the search for molecules with therapeutic potential against prion diseases.
机译:朊病毒蛋白(PRP)氨基酸序列的特异性变异是对朊病毒疾病易感性的关键决定因素。我们以前表明,当在小鼠中表达并表现出对各种不同起源和特征的各种传染朊病毒菌株的显性阴性保护作用,赋予CAIL特异性氨基酸取代赋予朊病毒疾病的抵抗力。在这里,我们表明,这种单一氨基酸变化的表达显着增加了表达群体族细胞朊病毒蛋白的转基因小鼠中的存活时间(prp(c)),其在用两个不同的朊病毒菌株接种后固有地容易被误用(cwd-血液菌株和自发起源的非典型菌株)。该氨基酸取代阻碍了双朊病毒菌株的繁殖,即使在PRP(c)的上下文中表达唯一易受各种朊病毒分离物的情况下表达。表达该取代的非接种小鼠体验了自发的朊病毒形成,但显示出与突变小鼠在接种的突变小鼠中观察到的存活时间的增加。我们的结果强调了该PRP变体在寻找具有治疗潜力患者疾病的分子中的重要性。

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