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Detection of RNA in the Plasma of Patients with Sporadic Creutzfeldt–Jakob Disease, Gerstmann–Straüssler Syndrome and Other Non-Transmissible Spongiform Encephalopathy Brain Disorders

机译:散发性Creutzfeldt–Jakob病,Gerstmann–Straüssler综合征和其他非传染性海绵状脑病脑病患者血浆中RNA的检测

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The infectious agent of transmissible spongiform encephalopathy (TSE) was assumed to be the aggregate of abnormal prion protein isoform (PrPsc). We observed that lowering the pH of 3% SDS-inoculated plasma or brain homogenate after PK digestion to 4.5 (acidic SDS condition) enabled to precipitate proteinase K-resistant prion protein (PrPres) in plasma as well as PrPres in the brain with synthetic poly-A RNA as affinity aggregate. Therefore, we determined if RNA molecules could be used for discriminating TSE patients from healthy individuals. We also examined the plasma of patients with classical Creutzfeldt–Jakob disease (CJD) and other brain disorders who were not diagnosed with TSE. The results indicated that RNA approximately 1.5–2.0 kb in length was commonly observed in the plasma of patients with brain disorders but was not detected in the plasma of healthy volunteers. Enhanced expression of RNA and its protection from endogenous nucleases might occur in the former group of patients. Moreover, we speculate that the non-transmissible neuronal disorders overlap with prion diseases.
机译:传染性海绵状脑病(TSE)的传染原被假定为abnormal病毒蛋白同工型异常(PrPsc)的聚集体。我们观察到,PK消化后,将接种3%SDS的血浆或大脑匀浆的pH降低至4.5(酸性SDS条件),可以使血浆中的蛋白酶K抗病毒蛋白(PrPres)沉淀,并通过合成的聚乳酸在大脑中沉淀PrPres -RNA作为亲和力聚集体。因此,我们确定了RNA分子是否可用于区分TSE患者和健康个体。我们还检查了未诊断为TSE的典型Creutzfeldt–Jakob病(CJD)和其他脑部疾病的患者的血浆。结果表明,在患有脑疾病的患者血浆中通常观察到大约1.5–2.0 kb的RNA,但在健康志愿者的血浆中未检测到。在前一组患者中可能会增强RNA的表达及其免受内源性核酸酶的保护。此外,我们推测不可传播的神经元疾病与病毒疾病重叠。

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