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溶瘤性单纯疱疹病毒对中性粒细胞的迁移、表型和抗原呈递能力及其获取非结构病毒蛋白能力的影响特征。

Characterization of the Impact of Oncolytic Vesicular Stomatitis Virus on the Trafficking, Phenotype, and Antigen Presentation Potential of Neutrophils and Their Ability to Acquire a Non-Structural Viral Protein.

机构信息

Department of Pathobiology, Ontario Veterinary College, University of Guelph, Guelph, ON N1G 2W1, Canada.

Department of Biomedical Sciences, Ontario Veterinary College, University of Guelph, Guelph, ON N1G 2W1, Canada.

出版信息

Int J Mol Sci. 2020 Sep 1;21(17):6347. doi: 10.3390/ijms21176347.

DOI:10.3390/ijms21176347
PMID:32882969
原文链接:https://pmc.ncbi.nlm.nih.gov/articles/PMC7570176/
Abstract

Neutrophils are innate leukocytes that mount a rapid response to invading pathogens and sites of inflammation. Although neutrophils were traditionally considered responders to bacterial infections, recent advances have demonstrated that they are interconnected with both viral infections and cancers. One promising treatment strategy for cancers is to administer an oncolytic virus to activate the immune system and directly lyse cancerous cells. A detailed characterization of how the innate immune system responds to a viral-based therapy is paramount in identifying its systemic effects. This study analyzed how administering the rhabdovirus vesicular stomatitis virus (VSV) intravenously at 1 × 10 PFU acutely influenced neutrophil populations. Bone marrow, blood, lungs, and spleen were acquired three- and 24-h after administration of VSV for analysis of neutrophils by flow cytometry. Infection with VSV caused neutrophils to rapidly egress from the bone marrow and accumulate in the lungs. A dramatic increase in immature neutrophils was observed in the lungs, as was an increase in the antigen presentation potential of these cells within the spleen. Furthermore, the potential for neutrophils to acquire viral transgene-encoded proteins was monitored using a variant of VSV that expressed enhanced green fluorescent protein (GFP). If an population of splenocytes were exposed to αCD3 and αCD28, a substantial proportion of the neutrophils would become GFP-positive. This suggested that the neutrophils could either acquire more virus-encoded antigens from infected splenocytes or were being directly infected. Five different dosing regimens were tested in mice, and it was determined that a single dose of VSV or two doses of VSV administered at a 24-h interval, resulted in a substantial proportion of neutrophils in the bone marrow becoming GFP-positive. This correlated with a decrease in the number of splenic neutrophils. Two doses administered at intervals longer than 24-h did not have these effects, suggesting that neutrophils became resistant to antigen uptake or direct infection with VSV beyond 24-h of activation. These findings implicated neutrophils as major contributors to oncolytic rhabdoviral therapies. They also provide several clear future directions for research and suggest that neutrophils should be carefully monitored during the development of all oncolytic virus-based treatment regimens.

摘要

中性粒细胞是先天白细胞,对入侵病原体和炎症部位迅速作出反应。尽管中性粒细胞传统上被认为是对细菌感染的反应者,但最近的进展表明,它们与病毒感染和癌症都有关联。癌症的一种有前途的治疗策略是给予溶瘤病毒以激活免疫系统并直接裂解癌细胞。详细描述先天免疫系统对基于病毒的治疗的反应对于确定其全身效应至关重要。本研究分析了静脉内给予 1×10 PFU 的弹状病毒水疱性口炎病毒 (VSV) 如何急性影响中性粒细胞群体。在给予 VSV 后 3 小时和 24 小时采集骨髓、血液、肺和脾,通过流式细胞术分析中性粒细胞。VSV 感染导致中性粒细胞迅速从骨髓迁出并积聚在肺部。在肺部观察到未成熟中性粒细胞的急剧增加,以及这些细胞在脾脏中的抗原呈递潜力增加。此外,使用表达增强型绿色荧光蛋白 (GFP) 的 VSV 变体监测中性粒细胞获得病毒转基因编码蛋白的潜力。如果将一群脾细胞暴露于 αCD3 和 αCD28,相当比例的中性粒细胞将变为 GFP 阳性。这表明中性粒细胞要么从感染的脾细胞中获得更多病毒编码的抗原,要么直接被感染。在小鼠中测试了五种不同的剂量方案,结果表明单次剂量的 VSV 或两次剂量的 VSV 间隔 24 小时给予,导致骨髓中的相当一部分中性粒细胞变为 GFP 阳性。这与脾中性粒细胞数量减少相关。间隔超过 24 小时给予两次剂量没有这些效果,这表明中性粒细胞对 VSV 的抗原摄取或直接感染变得具有抗性超过 24 小时的激活。这些发现将中性粒细胞牵连为溶瘤性弹状病毒治疗的主要贡献者。它们还为未来的研究提供了几个明确的方向,并表明在所有溶瘤病毒治疗方案的开发过程中应仔细监测中性粒细胞。

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