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Rapid amplification of prions from variant Creutzfeldt–Jakob disease cerebrospinal fluid

机译:快速变异的Creutzfeldt–Jakob病脑脊髓液中的病毒

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Human prion diseases constitute a group of infectious and invariably fatal neurodegenerative disorders associated with misfolding of the prion protein. Variant Creutzfeldt–Jakob disease (vCJD) is a zoonotic prion disease linked to oral exposure to the infectious agent that causes bovine spongiform encephalopathy (BSE) in cattle. The most recent case of definite vCJD was heterozygous (MV) at polymorphic codon 129 of the prion protein gene PRNP while all of the previous 177 definite or probable vCJD cases who underwent genetic analysis were methionine homozygous (MM). Retrospective prevalence studies conducted on lympho‐reticular tissue suggest that the number of asymptomatic vCJD carriers in the United Kingdom might be around 1 in 2000 people. In addition, there have been four known cases of the transmission of vCJD infection via blood transfusion. For these reasons, a sensitive, reliable, and fast diagnostic test is currently needed. We describe a rapid and highly sensitive seeding conversion assay that detects disease‐associated prion protein in the brain and cerebrospinal fluid in vCJD after 48–96 h of amplification, with 100% sensitivity and specificity. This method can amplify prions from definite, probable, and possible vCJD cases from patients who are either MM or MV at PRNP ‐codon 129.
机译:人类病毒疾病构成了与the病毒蛋白质错误折叠有关的一组感染性疾病,并总是致命性神经退行性疾病。变种克雅氏病(vCJD)是一种人畜共患性病毒病,与口服暴露于引起牛海绵状脑病(BSE)的传染原有关。最近的确定性vCJD病例是pr病毒蛋白基因PRNP多态密码子129处的杂合子(MV),而之前进行基因分析的177个确定性或可能的vCJD病例均为甲硫氨酸纯合子(MM)。对淋巴网状组织进行的回顾性患病率研究表明,英国无症状vCJD携带者的数量可能约为2000人中的1人。另外,已经有四个已知案例通过输血传播vCJD感染。由于这些原因,当前需要灵敏,可靠且快速的诊断测试。我们描述了一种快速,高度灵敏的接种转化试验,该试验可在扩增48-96小时后以100%的灵敏度和特异性检测vCJD中大脑和脑脊液中与疾病相关的pr病毒蛋白。这种方法可以从PRNP密码子129的MM或MV患者的确定的,可能的和可能的vCJD病例中扩增病毒。

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