Differentiation of highly pathogenic strains of human JC polyomavirus in neurological patients by next generation sequencing

IF 4 3区 医学 Q2 VIROLOGY
Eeva Auvinen , Anni Honkimaa , Pia Laine , Sara Passerini , Ugo Moens , Valeria Pietropaolo , Mika Saarela , Leena Maunula , Laura Mannonen , Olli Tynninen , Hannu Haapasalo , Tuomas Rauramaa , Petri Auvinen , Hanna Liimatainen
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引用次数: 0

Abstract

Background

JC polyomavirus (JCPyV) persists asymptomatic in more than half of the human population. Immunocompromising conditions may cause reactivation and acquisition of neurotropic rearrangements in the viral genome, especially in the non-coding control region (NCCR). Such rearranged JCPyV strains are strongly associated with the development of progressive multifocal leukoencephalopathy (PML).

Methods

Using next-generation sequencing (NGS) and bioinformatics tools, the NCCR was characterized in cerebrospinal fluid (CSF; N = 21) and brain tissue (N = 16) samples from PML patients (N = 25), urine specimens from systemic lupus erythematosus patients (N = 2), brain tissue samples from control individuals (N = 2) and waste-water samples (N = 5). Quantitative PCR was run in parallel for diagnostic PML samples.

Results

Archetype NCCR (i.e. ABCDEF block structure) and archetype-like NCCR harboring minor mutations were detected in two CSF samples and in one CSF sample and in one tissue sample, respectively. Among samples from PML patients, rearranged NCCRs were found in 8 out of 21 CSF samples and in 14 out of 16 brain tissue samples. Complete or partial deletion of the C and D blocks was characteristic of most rearranged JCPyV strains. From ten CSF samples and one tissue sample NCCR could not be amplified.

Conclusions

Rearranged NCCRs are predominant in brain tissue and common in CSF from PML patients. Extremely sensitive detection and identification of neurotropic viral populations in CSF or brain tissue by NGS may contribute to early and accurate diagnosis, timely intervention and improved patient care.

利用新一代测序技术区分神经系统患者体内的人类 JC 多瘤病毒高致病性毒株
背景JC多瘤病毒(JCPyV)在一半以上的人群中无症状。免疫力低下可能会导致病毒重新活化,并在病毒基因组中,尤其是在非编码控制区(NCCR)中获得神经性重排。这种重排的 JCPyV 株与进行性多灶性白质脑病(PML)的发生密切相关。方法利用新一代测序(NGS)和生物信息学工具,对 PML 患者(25 例)的脑脊液(CSF;21 例)和脑组织(16 例)样本、系统性红斑狼疮患者(2 例)的尿液样本、对照组(2 例)的脑组织样本和废水样本(5 例)中的 NCCR 进行表征。结果分别在两份 CSF 样本、一份 CSF 样本和一份组织样本中检测到原型 NCCR(即 ABCDEF 块状结构)和携带微小突变的原型样 NCCR。在 PML 患者的样本中,21 份 CSF 样本中有 8 份发现了重排的 NCCR,16 份脑组织样本中有 14 份发现了重排的 NCCR。C和D区块的完全或部分缺失是大多数重排 JCPyV 株系的特征。结论重排的 NCCR 主要存在于 PML 患者的脑组织和 CSF 中。通过 NGS 极其灵敏地检测和鉴定 CSF 或脑组织中的致神经病毒群可能有助于早期准确诊断、及时干预和改善患者护理。
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来源期刊
Journal of Clinical Virology
Journal of Clinical Virology 医学-病毒学
CiteScore
22.70
自引率
1.10%
发文量
149
审稿时长
24 days
期刊介绍: The Journal of Clinical Virology, an esteemed international publication, serves as the official journal for both the Pan American Society for Clinical Virology and The European Society for Clinical Virology. Dedicated to advancing the understanding of human virology in clinical settings, the Journal of Clinical Virology focuses on disseminating research papers and reviews pertaining to the clinical aspects of virology. Its scope encompasses articles discussing diagnostic methodologies and virus-induced clinical conditions, with an emphasis on practicality and relevance to clinical practice. The journal publishes on topics that include: • new diagnostic technologies • nucleic acid amplification and serologic testing • targeted and metagenomic next-generation sequencing • emerging pandemic viral threats • respiratory viruses • transplant viruses • chronic viral infections • cancer-associated viruses • gastrointestinal viruses • central nervous system viruses • one health (excludes animal health)
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