PD-1 AND Tim-3 Expression on different subpopulations of monocytes in chronic often recurrent herpesvirus infection

Ivan M. Rashchupkin, I. Meledina, M. Kotova, O. Zheltova
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Abstract

More than half of the world’s population is infected with the herpes simplex virus. In most cases, infection is not accompanied by symptoms, but in some people the disease occurs as a chronic infection with frequent and severe relapses. One of the most likely reasons for this may be a dysregulation of the immune system. In recent years, the role of checkpoint molecules, in particular PD-1 and Tim-3, in the regulation of the immune response and the functions of immunocompetent cells has been actively studied. Activation of PD-1 and Tim-3 on T cells has previously been shown to suppress the immune response. PD-1 and Tim-3 are also expressed on other immune cells, in particular monocytes. However, the expression of these molecules on monocytes during chronic viral infections has not been previously studied. The study was aimed at assessing the level of PD-1 and Tim-3 expression on various populations of monocytes in patients with chronic often recurrent herpesvirus infection. Twenty-six patients were recruited into the study. All patients received antiviral and immunomodulatory therapy in the immunological department. The number of classical, intermediate, and non-classical monocytes and the expression of PD-1 and Tim-3 on monocytes, were assessed by flow cytometry before and after the therapy. Monocytes were isolated from peripheral blood, and subpopulations were divided according to the level of expression of CD14 and CD16. In patients with herpes, a reduced number of monocytes was observed in comparison with healthy donors. The relative number of PD-1-positive monocytes, the mean fluorescence intensity of PD-1 and Tim-3, and the number of double-positive cells were reduced in herpes patients in all three monocyte subpopulations examined. Three months after therapy, the response to the therapy was assessed; patients who did not have a single recurrence of herpes within 3 months were considered to respond. Responding patients had a lower initial content of double-positive cells among intermediate and non-classical monocytes. The decrease in the level of PD-1 and Tim-3 positive monocytes during herpesvirus infection revealed in the present study may indicate the involvement of monocytes deficient in the expression of checkpoint molecules in the pathogenesis of the disease.
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慢性经常复发性疱疹病毒感染中不同亚群单核细胞上的 PD-1 和 Tim-3 表达
世界上有一半以上的人口感染了单纯疱疹病毒。在大多数情况下,感染并不伴有症状,但在一些人身上,这种疾病是一种慢性感染,复发频繁且严重。其中一个最可能的原因可能是免疫系统失调。近年来,人们积极研究了检查点分子,特别是 PD-1 和 Tim-3 在调节免疫反应和免疫功能细胞功能中的作用。先前的研究表明,激活 T 细胞上的 PD-1 和 Tim-3 可抑制免疫反应。PD-1 和 Tim-3 也在其他免疫细胞,特别是单核细胞上表达。但在慢性病毒感染期间,这些分子在单核细胞上的表达情况以前还没有研究过。这项研究旨在评估慢性经常复发性疱疹病毒感染患者各种单核细胞群中 PD-1 和 Tim-3 的表达水平。研究共招募了 26 名患者。所有患者都在免疫科接受了抗病毒和免疫调节治疗。通过流式细胞术评估了治疗前后经典、中间和非经典单核细胞的数量以及单核细胞上 PD-1 和 Tim-3 的表达。从外周血中分离出单核细胞,并根据 CD14 和 CD16 的表达水平划分亚群。与健康供体相比,疱疹患者的单核细胞数量有所减少。在疱疹患者的所有三个单核细胞亚群中,PD-1 阳性单核细胞的相对数量、PD-1 和 Tim-3 的平均荧光强度以及双阳性细胞的数量都有所减少。治疗三个月后,对治疗反应进行评估;三个月内未复发一次疱疹的患者被视为有反应。应答患者的中型和非典型单核细胞中双阳性细胞的初始含量较低。本研究发现,在疱疹病毒感染期间,PD-1 和 Tim-3 阳性单核细胞水平下降,这可能表明缺乏检查点分子表达的单核细胞参与了疾病的发病机制。
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