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单纯疱疹病毒 1 病毒发病机制中的病毒 microRNAs。

Viral MicroRNAs in Herpes Simplex Virus 1 Pathobiology.

机构信息

Department of Periodontics, College of Dentistry, University of Illinois Chicago, Chicago, Illinois 60607, USA.

Department of Ophthalmology and Visual Sciences, Medical Center, University of Illinois Chicago, Chicago, Illinois 60607, USA.

出版信息

Curr Pharm Des. 2024;30(9):649-665. doi: 10.2174/0113816128286469240129100313.

DOI:10.2174/0113816128286469240129100313
PMID:38347772
Abstract

(Herpes simplex virus type 1 [HSV-1]) infects millions of people globally, manifesting as vesiculo-ulcerative lesions of the oral or genital mucosa. After primary infection, the virus establishes latency in the peripheral neurons and reactivates sporadically in response to various environmental and genetic factors. A unique feature of herpesviruses is their ability to encode tiny noncoding RNAs called microRNA (miRNAs). encodes eighteen miRNA precursors that generate twentyseven different mature miRNA sequences. Unique miRNAs repertoire is expressed in lytic and latent stages and exhibits expressional disparity in various cell types and model systems, suggesting their key pathological functions. This review will focus on elucidating the mechanisms underlying the regulation of host-virus interaction by HSV-1 encoded viral miRNAs. Numerous studies have demonstrated sequence- specific targeting of both viral and host transcripts by miRNAs. While these noncoding RNAs predominantly target viral genes involved in viral life cycle switch, they regulate host genes involved in antiviral immunity, thereby facilitating viral evasion and lifelong viral persistence inside the host. Expression of miRNAs has been associated with disease progression and resolution. Systemic circulation and stability of viral miRNAs compared to viral mRNAs can be harnessed to utilize their potential as diagnostic and prognostic markers. Moreover, functional inhibition of these enigmatic molecules may allow us to devise strategies that have therapeutic significance to contain infection.

摘要

(单纯疱疹病毒 1[HSV-1]) 感染全球数百万人,表现为口腔或生殖器黏膜的水疱 - 溃疡性病变。原发感染后,病毒在外周神经元中潜伏,并因各种环境和遗传因素而间歇性激活。疱疹病毒的一个独特特征是它们能够编码称为 microRNA (miRNA) 的微小非编码 RNA。 编码十八个 miRNA 前体,生成二十七个不同的成熟 miRNA 序列。独特的 miRNA 谱在裂解和潜伏阶段表达,并在不同的细胞类型和模型系统中表现出表达差异,表明它们具有关键的病理功能。本综述将重点阐述 HSV-1 编码的病毒 miRNA 调节宿主 - 病毒相互作用的机制。许多研究已经证明了 miRNA 对病毒和宿主转录物的序列特异性靶向。虽然这些非编码 RNA 主要靶向病毒基因参与病毒生命周期转换,但它们调节宿主基因参与抗病毒免疫,从而促进病毒逃逸和宿主内终生病毒持续存在。miRNA 的表达与疾病进展和消退有关。与病毒 mRNA 相比,病毒 miRNA 的系统循环和稳定性可用于利用其作为诊断和预后标志物的潜力。此外,这些神秘分子的功能抑制可能使我们能够设计具有治疗意义的策略来控制 感染。

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