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Viral Metagenomics on Cerebrospinal Fluid

机译:脑脊液的病毒基因组学

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摘要

Identifying the causative pathogen in central nervous system (CNS) infections is crucial for patient management and prognosis. Many viruses can cause CNS infections, yet screening for each individually is costly and time-consuming. Most metagenomic assays can theoretically detect all pathogens, but often fail to detect viruses because of their small genome and low viral load. Viral metagenomics overcomes this by enrichment of the viral genomic content in a sample. VIDISCA-NGS is one of the available workflows for viral metagenomics, which requires only a small input volume and allows multiplexing of multiple samples per run. The performance of VIDISCA-NGS was tested on 45 cerebrospinal fluid (CSF) samples from patients with suspected CNS infections in which a virus was identified and quantified by polymerase chain reaction. Eighteen were positive for an RNA virus, and 34 for a herpesvirus. VIDISCA-NGS detected all RNA viruses with a viral load >2 × 104 RNA copies/mL (n = 6) and 8 of 12 of the remaining low load samples. Only one herpesvirus was identified by VIDISCA-NGS, however, when withholding a DNase treatment, 11 of 18 samples with a herpesvirus load >104 DNA copies/mL were detected. Our results indicate that VIDISCA-NGS has the capacity to detect low load RNA viruses in CSF. Herpesvirus DNA in clinical samples is probably non-encapsidated and therefore difficult to detect by VIDISCA-NGS.
机译:识别中枢神经系统(CNS)感染的病原体对于患者管理和预后至关重要。许多病毒可以引起CNS感染,但是对每个病毒进行单独的筛查既昂贵又费时。从理论上讲,大多数宏基因组测定法可以检测所有病原体,但由于其基因组小和病毒载量低,通常无法检测到病毒。病毒宏基因组学通过丰富样品中病毒基因组含量来克服这一问题。 VIDISCA-NGS是病毒宏基因组学的可用工作流程之一,仅需少量的输入量,并且允许每次运行多样品的多路复用。 VIDISCA-NGS的性能在来自可疑CNS感染患者的45例脑脊液(CSF)样本中进行了测试,其中通过聚合酶链反应鉴定和定量了病毒。 RNA病毒阳性18例,疱疹病毒34例。 VIDISCA-NGS检测到所有病毒载量> 2×10 4 RNA拷贝/ mL(n = 6)的RNA病毒,其余12个低载量样本中有8个。 VIDISCA-NGS仅鉴定出一种疱疹病毒,但是,在不进行DNase处理时,检测到18例疱疹病毒载量大于10 4 DNA拷贝/ mL的样品中有11个。我们的结果表明,VIDISCA-NGS具有检测CSF中低负荷RNA病毒的能力。临床样品中的疱疹病毒DNA可能没有被衣壳化,因此很难通过VIDISCA-NGS进行检测。

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