Department of Neurology, University of Colorado Anschutz Medical Campus, Aurora, Colorado, USA.
Department of Biomedical and Health Sciences, University of Vermont, Burlington, Vermont, USA.
J Virol. 2024 Aug 20;98(8):e0084824. doi: 10.1128/jvi.00848-24. Epub 2024 Jul 25.
Varicella zoster virus (VZV) reactivates from ganglionic sensory neurons to produce herpes zoster (shingles) in a unilateral dermatomal distribution, typically in the thoracic region. Reactivation not only heightens the risk of stroke and other neurological complications but also increases susceptibility to co-infections with various viral and bacterial pathogens at sites distant from the original infection. The mechanism by which VZV results in complications remote from the initial foci remains unclear. Small extracellular vesicles (sEVs) are membranous signaling structures that can deliver proteins and nucleic acids to modify the function of distal cells and tissues during normal physiological conditions. Although viruses have been documented to exploit the sEV machinery to propagate infection, the role of non-infectious sEVs released from VZV-infected neurons in viral spread and disease has not been studied. Using multi-omic approaches, we characterized the content of sEVs released from VZV-infected human sensory neurons (VZV sEVs). One viral protein was detected (immediate-early 62), as well as numerous immunosuppressive and vascular disease-associated host proteins and miRNAs that were absent in sEVs from uninfected neurons. Notably, VZV sEVs are non-infectious yet transcriptionally altered primary human cells, suppressing the antiviral type 1 interferon response and promoting neuroinvasion of a secondary pathogen . These results challenge our understanding of VZV infection, proposing that the virus may contribute to distant pathologies through non-infectious sEVs beyond the primary infection site. Furthermore, this study provides a previously undescribed immune-evasion mechanism induced by VZV that highlights the significance of non-infectious sEVs in early VZV pathogenesis.
Varicella zoster virus (VZV) is a ubiquitous human virus that predominantly spreads by direct cell-cell contact and requires efficient and immediate host immune evasion strategies to spread. The mechanisms of immune evasion prior to virion entry have not been fully elucidated and represent a critical gap in our complete understanding of VZV pathogenesis. This study describes a previously unreported antiviral evasion strategy employed by VZV through the exploitation of the infected host cell's small extracellular vesicle (sEV) machinery. These findings suggest that non-infectious VZV sEVs could travel throughout the body, affecting cells remote from the site of infection and challenging the current understanding of VZV clinical disease, which has focused on local effects and direct infection. The significance of these sEVs in early VZV pathogenesis highlights the importance of further investigating their role in viral spread and secondary disease development to reduce systemic complications following VZV infections.
水痘带状疱疹病毒(VZV)从神经节感觉神经元中激活,以单侧皮节分布的形式产生带状疱疹(带状疱疹),通常在胸部区域。病毒激活不仅会增加中风和其他神经并发症的风险,还会增加与原始感染部位远处的各种病毒和细菌病原体的合并感染的易感性。VZV 导致远离初始病灶的并发症的机制尚不清楚。小细胞外囊泡(sEVs)是膜性信号结构,可以在正常生理条件下将蛋白质和核酸传递到远处的细胞和组织,以改变其功能。尽管已经有文献记录表明病毒利用 sEV 机制来传播感染,但从 VZV 感染神经元释放的非感染性 sEVs 在病毒传播和疾病中的作用尚未得到研究。使用多组学方法,我们对 VZV 感染的人感觉神经元释放的 sEVs 的内容进行了表征。检测到一种病毒蛋白(早期 62),以及许多免疫抑制和血管疾病相关的宿主蛋白和 miRNA,这些在未感染神经元的 sEVs 中不存在。值得注意的是,VZV sEVs 是非感染性的,但可改变原发性人细胞的转录,抑制抗病毒 1 型干扰素反应,并促进二次病原体的神经入侵。这些结果挑战了我们对 VZV 感染的理解,提出病毒可能通过原发性感染部位以外的非感染性 sEVs 导致远处病变。此外,这项研究提供了 VZV 诱导的以前未描述的免疫逃避机制,突出了非感染性 sEVs 在 VZV 早期发病机制中的重要性。
水痘带状疱疹病毒(VZV)是一种普遍存在的人类病毒,主要通过直接细胞-细胞接触传播,需要有效的即时宿主免疫逃避策略来传播。在病毒进入之前的免疫逃避机制尚未完全阐明,这是我们对 VZV 发病机制全面理解的一个关键空白。本研究描述了 VZV 利用受感染宿主细胞的小细胞外囊泡(sEV)机制的一种以前未报告的抗病毒逃避策略。这些发现表明,非感染性 VZV sEVs 可以在全身传播,影响感染部位以外的细胞,并挑战了当前对 VZV 临床疾病的理解,即主要关注局部影响和直接感染。这些 sEVs 在 VZV 早期发病机制中的重要性突出表明,需要进一步研究它们在病毒传播和继发疾病发展中的作用,以减少 VZV 感染后的全身并发症。
