Proinflammatory cytokines VEGFA, IL-6, IL-8 as markers of hepatotoxicity after COVID-19

M. A. Urevskii, L. V. Ilmukhina, Ya.E. Saranskaya, A. A. Lapshin, R. R. Gafurova
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Abstract

The mechanism of hepatocellular liver damage after COVID-19 is a multifactorial process. The most widely discussed causes are cytolytic liver damage due to the inflammatory response after COVID-19, drug-induced hepatotoxicity and direct cytotoxic effect of the virus. There are observations that SARSCoV-2 infection causes hepatitis B virus reactivation, but little has been described about the interaction between hepatitis C virus and SARS-CoV-2. The course of coronavirus infection is associated with marked expression of proinflammatory cytokines, participants in the multisystem inflammatory response, IL-1β, IL-6, IL-8, IL-18, MCP-1, TNFα, which contribute significantly to the observed early and late liver function impairment. The aim of the study was to evaluate the role of proinflammatory cytokines (VEGFA, IL-8, IL-6, MCP-1, TNFα, IL-18) as additional markers of hepatotoxicity after COVID-19. The study was performed between March and August 2022. Patients were divided into 2 groups: Group 1 – with increased aminotransferases against the background of treatment from COVID-19 and/or in the following 3-6 months after the disease without viral liver damage (n = 42), Group 2 – patients with co-infection (chronic viral hepatitis C (HCV) and COVID-19 (n = 26). The levels of cytokines – VEGF-A, IL-6, IL-8, MCP-1, IL-18, TNFα in blood serum were estimated by enzyme immunoassay method. Statistical analysis was performed using StatTech v. 3.1.4. The results of the study revealed a comparable increase in the level of transaminases and C-reactive protein in both groups, significantly different from the reference values. Direct correlations of moderate strength (linear Spearman correlation) were found between the following cytokines: TNFα-MCP-1 (R = 0.559; p = 0.001), TNFα-VEGFA (R = 0.400; p = 0.002), TNFα-IL-6 (R = 0.503; p = 0.001). We diagnosed a significant increase in serum VEGFA levels in group 1 patients (hepatotoxicity after COVID-19) (Me (Q0.25-Q0.75): 522 (250 to 1002), p = 0.001) and in group 2 patients (HCV + COVID-19) (Me 1196, Q0.25-Q0.75: (73 to 432). Similar trend with the level of IL-6, IL-8, exceeding the values of cytokines in healthy donors and significantly higher than in group 2 patients. Identified correlations between inflammatory cytokines prove unidirectional changes in the functioning of the regulatory network controlling immune virus-induced reactions.
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促炎因子VEGFA、IL-6、IL-8作为COVID-19后肝毒性的标志物
新冠肺炎后肝细胞性肝损伤的机制是一个多因素的过程。最广泛讨论的原因是COVID-19后炎症反应引起的细胞溶解性肝损伤、药物诱导的肝毒性和病毒的直接细胞毒性作用。有观察表明,SARS-CoV-2感染可引起乙型肝炎病毒再激活,但关于丙型肝炎病毒与SARS-CoV-2之间相互作用的描述很少。冠状病毒感染过程中,促炎因子、多系统炎症反应参与者、IL-1β、IL-6、IL-8、IL-18、MCP-1、TNFα的显著表达与早期和晚期肝功能损害相关。本研究的目的是评估促炎细胞因子(VEGFA、IL-8、IL-6、MCP-1、TNFα、IL-18)作为COVID-19后肝毒性的附加标志物的作用。该研究于2022年3月至8月进行。患者分为2组:1组-在COVID-19治疗背景下转氨酶升高和/或在疾病后3-6个月内无病毒性肝损害(n = 42), 2组-合并感染(慢性病毒性丙型肝炎(HCV)和COVID-19患者(n = 26)。采用酶免疫分析法测定血清中VEGF-A、IL-6、IL-8、MCP-1、IL-18、tnf - α等细胞因子水平。使用StatTech v. 3.1.4进行统计分析。研究结果显示,两组患者的转氨酶和c反应蛋白水平均有相当程度的升高,与参考值有显著差异。以下细胞因子与TNFα-MCP-1呈中等强度的直接相关(线性Spearman相关):TNFα-MCP-1 (R = 0.559;p = 0.001), tnf - α- vegfa (R = 0.400;p = 0.002), TNFα-IL-6 (R = 0.503;P = 0.001)。我们诊断出第1组患者(COVID-19后肝毒性)(Me (Q0.25-Q0.75): 522(250至1002),p = 0.001)和第2组患者(HCV + COVID-19) (Me 1196, Q0.25-Q0.75: 73至432)血清VEGFA水平显著升高。IL-6、IL-8水平与健康供者相似,均超过细胞因子水平,且明显高于2组。已确定的炎症细胞因子之间的相关性证明了控制免疫病毒诱导反应的调节网络功能的单向变化。
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来源期刊
Medical Immunology (Russia)
Medical Immunology (Russia) Medicine-Immunology and Allergy
CiteScore
0.70
自引率
0.00%
发文量
88
审稿时长
12 weeks
期刊介绍: The journal mission is to promote scientific achievements in fundamental and applied immunology to various medical fields, the publication of reviews, lectures, essays by leading domestic and foreign experts in the field of fundamental and experimental immunology, clinical immunology, allergology, immunodiagnostics and immunotherapy of infectious, allergy, autoimmune diseases and cancer.
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