重组干扰素α2b对CD16<sup>+</sup>INFα/βR1<sup>-</sup> cd116 <sup>+</sup>; CD16<sup>+</sup>INFα/βR1<sup>+</sup>CD119<sup>-</sup>covid后综合征和疱疹病毒感染患者的中性粒细胞亚群

M. G. Atazhakhova, Irina V. Nesterova, G. A. Chudilova, V. A. Matushkina, S. V. Kovaleva, V. N. Chapurina
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引用次数: 0

摘要

covid后综合征(PCS)是一种多系统炎症,表现为慢性疲劳综合征(CFS)和认知障碍(CD),并伴有慢性疱疹病毒感染(HVI)的再激活。PCS的表现需要研究与IFN产生和中性粒细胞(NG)受体功能相关的分子机制,这是相关的,并促进了PCS患者免疫治疗策略的探索。我们的目的是研究重组干扰素2b (recIFN2b)对covid后综合征和疱疹病毒感染患者CD16+IFN/R1-CD119+、CD16+IFN/R1 +CD119+亚群表型和NG功能活性的体外影响。材料和方法:研究组1 (SG1)为45例PCS合并HVI (HSV 1、EBV、HHV6、CMV)患者,年龄24-60岁。采用计分量表进行问卷调查,评估PCS症状的严重程度。我们在研究组1a (SG1a)中研究了NG亚群的含量和表型,即CD16+IFN/R1-CD119+, CD16+IFN/R1+CD119-, CD16+IFN/R1+CD119+亚群,在体外与recIFN2b (50 IU/ L, 60分钟,37℃)孵育前后NG的吞噬和NADPH氧化酶功能。对照组(CG)由30名志愿者组成,他们在新冠肺炎前接受了检查。结果:我们发现SG1混合HVI患者的CFS和CD的临床表现比单一HVI患者更明显。所有受体在CD16+IFN/R1+CD119-NG和CD16+IFN/R1- CD119-NG上的表达密度均有所增加,这表明NG的激活伴随着细胞毒性或NETosis的启动,吞噬功能下降,NADPH氧化酶活性增强伴随着SG1中NG储备能力的消耗。我们已经在体外获得了一些关于recIFN2b的积极作用(SG1a)的数据,例如,在CD16+IFN/R1+CD119-亚群中,降低CD16表达密度和增强IFN/R1受体表达。在CD16+IFN/R1-CD119+亚群中,我们发现MFI CD16和MFI CD119受体持续增加,NG吞噬功能缺陷恢复,NADPH氧化酶活性过度降低。结论:recIFN2b对PCS患者NG功能缺陷的积极影响提示,使用基于recIFN2b的药物进行免疫治疗,结合高活性抗氧化剂治疗各种PCS表现,包括CFS、CD、HVI,从而可能确保免疫系统抗病毒和调节机制的充分发挥作用。
本文章由计算机程序翻译,如有差异,请以英文原文为准。
Positive effects of recombinant interferon α2b on the phenotype of CD16<sup>+</sup>INFα/βR1<sup>-</sup>CD119<sup>+</sup>, CD16<sup>+</sup>INFα/βR1<sup>+</sup>CD119<sup>-</sup> neutrophil granulocyte subset in patients with post-COVID syndrome and herpesvirus infections
Post-COVID syndrome (PCS) is a multisystem inflammatory condition with manifestations of chronic fatigue syndrome (CFS) and cognitive disorders (CD), along with reactivation of chronic herpesvirus infections (HVI). The PCS manifestations require studying the molecular mechanisms associated with the production of IFN and receptor functions of neutrophil granulocytes (NG), which is relevant and promotes the search for immunotherapeutic strategies in patients with PCS. Our objective was to study the in vitro effects of recombinant interferon 2b (recIFN2b) on the phenotype of CD16+IFN/R1-CD119+, CD16+IFN/ R1+CD119+ subsets and functional activity of NG in patients with post-COVID syndrome and herpesvirus infections. Materials and methods: 45 patients (24-60 years old) with PCS and HVI (HSV 1, EBV, HHV6, CMV) comprised the study group 1 (SG1). A questionnaire was conducted to assess the severity of PCS symptoms using a point scale. We performed a study of the content and phenotype of NG subsets, i.e., the CD16+IFN/R1-CD119+, CD16+IFN/R1+CD119-, CD16+IFN/R1+CD119+ subpopulation, phagocytic and NADPH oxidase function of NG before and after in vitro incubation with recIFN2b (50 IU/ L, for 60 min, at 37 C) in the study group 1a (SG1a). The comparison group (CG) of 30 volunteers examined during the pre-COVID period. Results: We revealed more pronounced clinical manifestations of CFS and CD in SG1 patients with mixed HVI, than in mono-HVI cases. Increased expression density of all receptors was registered on CD16+IFN/R1+CD119-NG and CD16+IFN/R1-CD119+ NG, thus suggesting the NG activation with initiation of cytotoxicity or NETosis, a decrease in phagocytic function and intensity of NADPH oxidase activity with depletion of NG reserve capacity in SG1. We have obtained some data on the positive effect of recIFN2b in vitro (SG1a), e.g., decreased CD16 expression density and enhancement of IFN/R1 receptor expression in the CD16+IFN/R1+CD119- subset. In the CD16+IFN/R1-CD119+ subset, we have found persistence of increased MFI CD16 and MFI CD119 receptors, restoration of defective NG phagocytic function and reduced excessive activity of NADPH oxidases. Conclusion: The positive effects of the recIFN2b influence on deficient function of NG in PCS patients suggest an oppoptunity of using immunotherapy with a recIFN2b-based drug, combined with highly active antioxidants for treatment of various PCS manifestations including CFS, CD, HVI, thus, probably, ensuring adequate functioning of antiviral and regulatory mechanisms of the immune system.
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