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Previremic Identification of Ebola or Marburg Virus Infection Using Integrated Host-Transcriptome and Viral Genome Detection

机译:使用整合宿主转录组和病毒基因组检测急性鉴定埃博拉或马尔堡病毒感染

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摘要

Outbreaks of filoviruses, such as those caused by the Ebola (EBOV) and Marburg (MARV) virus, are difficult to detect and control. The initial clinical symptoms of these diseases are nonspecific and can mimic other endemic pathogens. This makes confident diagnosis based on clinical symptoms alone impossible. Molecular diagnostics for these diseases that rely on the detection of viral RNA in the blood are only effective after significant disease progression. As an approach to identify these infections earlier in the disease course, we tested the effectiveness of viral RNA detection combined with an assessment of sentinel host mRNAs that are upregulated following filovirus infection. RNAseq analysis of EBOV-infected nonhuman primates identified host RNAs that are upregulated at early stages of infection. NanoString probes that recognized these host-response RNAs were combined with probes that recognized viral RNA and were used to classify viral infection both prior to viremia and postviremia. This approach was highly successful at identifying samples from nonhuman primate subjects and correctly distinguished the causative agent in a previremic stage in 10 EBOV and 5 MARV samples. This work suggests that unified host response/viral fingerprint assays can enable diagnosis of disease earlier than testing for viral nucleic acid alone, which could decrease transmission events and increase therapeutic effectiveness.
机译:爆发的泌尿病毒,例如由埃博拉(EBOV)和Marburg(Marv)病毒引起的那些难以检测和控制。这些疾病的初始临床症状是非特异性的,可以模仿其他地方性病原体。这使得基于临床症状的自信诊断是不可能的。这些疾病的分子诊断依赖于血液中病毒RNA检测的疾病仅在显着的疾病进展后才能有效。作为在疾病课程中鉴定这些感染的方法,我们测试了病毒RNA检测的有效性结合了寄生宿主MRNA的评估,该宿主MRNA在泌尿病毒感染后上调。 EBOV感染的非人的RNA态分析鉴定在感染的早期阶段上调的宿主RNA。将这些宿主反应RNA认识到这些宿主响应RNA的纳米过度探针与识别病毒RNA的探针组合,并用于在病毒血症和后血症之前对病毒感染进行分类。这种方法在鉴定非人类气激发受试者的样本并正确地区分初级阶段的致病剂在10个EBOV和5个MARV样品中的致病剂。这项工作表明,统一宿主响应/病毒指纹测定可以比单独对病毒核酸的测试诊断,这可能降低传动事件并提高治疗效果。

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