Production of some cytokines as a reflection of various immunoregulatory mechanisms in post-covid myocarditis

Russian Journal of Infection and Immunity Pub Date : 2024-07-28 DOI:10.15789/2220-7619-pos-16582

Oxana V. Moskaletc

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Abstract

Currently, the problem of persistent myocardial damage in patients who have had COVID-19 has become one of the most pressing in the practice of cardiologists. The main mechanisms of the pathogenesis of post-COVID myocarditis are associated with a violation of immunoregulation caused by long-term persistence of the virus in the heart muscle and the launch of autoimmune processes that can lead to myocardial remodeling, the formation of myocardiosclerosis and the development of heart failure or arrhythmia. The purpose of this study was to assess the dynamics of the production of certain cytokines (IFNg, IL-4, IL-17А), which may indirectly reflect the activation of various immune response pathways in patients with post-COVID myocarditis, depending on the duration of the disease and the degree of heart failure. The study included 32 patients with post-COVID myocarditis, 36 patients with myocardial cardiosclerosis, and 10 apparently healthy individuals. It was found that in all patients with post-COVID myocarditis, the content of IFNg, IL-4, IL-17А in the blood serum was higher than in patients with myocardial cardiosclerosis (p 0.001; p 0.05; p 0.01, respectively) and conditionally healthy individuals (p 0.001; p 0.01; p 0.001, respectively). Compared with the group of patients with no or moderate severity of symptoms of heart failure (functional class 0–II), those with more severe heart failure (functional class III) had a higher level of interferon gamma (p 0.05). When comparing the results obtained with similar indicators in patients with myocardial cardiosclerosis who have the same degree of heart failure, no statistically significant differences were obtained. The maximum content of IFNg in post-COVID myocarditis was observed in the 2nd week of the disease (p 0.001 compared with the control group); then its level gradually decreased and by the end of the 2nd month there were no longer any significant differences. The opposite trend was observed in relation to the content of IL-4 and IL-17А: in the first two weeks, no statistically significant differences were detected with the control group, but then their content increased quite quickly (p 0.001 compared with the control group by the end of the first month of the disease) and continued to remain the same high until the end of the 2nd month. Thus, monitoring the content of IFNg, IL-4, IL-17А in blood serum can to some extent provide an idea of the sequence of development of the immune response in post-COVID myocarditis. An increase in IFNg levels in the early stages of the disease is probably associated with an increase in the manifestations of heart failure. Th17-mediated mechanisms may be involved in the process of myocardial remodeling resulting in myocardial cardiosclerosis.

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一些细胞因子的产生反映了包虫后心肌炎的各种免疫调节机制

目前，COVID-19 患者心肌持续受损的问题已成为心脏病专家临床工作中最紧迫的问题之一。COVID 后心肌炎的主要发病机制与病毒在心肌中长期存留引起的免疫调节失调以及自身免疫过程的启动有关，这些免疫过程可导致心肌重塑、心肌硬化的形成以及心力衰竭或心律失常的发生。本研究的目的是评估某些细胞因子（IFNg、IL-4、IL-17А）的产生动态，这些细胞因子可间接反映 COVID 后心肌炎患者各种免疫反应途径的激活情况，具体取决于病程长短和心衰程度。研究对象包括 32 名 COVID 后心肌炎患者、36 名心肌硬化症患者和 10 名表面健康的人。研究发现，所有 COVID 后心肌炎患者血清中 IFNg、IL-4、IL-17А 的含量均高于心肌硬化患者（分别为 p 0.001；p 0.05；p 0.01）和条件健康者（分别为 p 0.001；p 0.01；p 0.001）。与无心力衰竭症状或心力衰竭症状中等程度（功能分级 0-II）的患者组相比，心力衰竭症状较重（功能分级 III）的患者的γ干扰素水平较高（P 0.05）。与心肌梗塞患者的类似指标相比，心衰程度相同的心肌梗塞患者的结果在统计学上没有显著差异。COVID 后心肌炎患者的 IFNg 含量在病程的第 2 周达到最高值（与对照组相比，P 0.001），然后逐渐下降，到第 2 个月末，不再有任何显著差异。IL-4和IL-17А的含量则呈现出相反的趋势：在前两周，与对照组相比没有发现明显的统计学差异，但随后它们的含量迅速增加（在疾病的第一个月结束时，与对照组相比，p 0.001），并在第二个月结束前一直保持同样的高水平。因此，监测血清中 IFNg、IL-4、IL-17А 的含量可在一定程度上了解 COVID 后心肌炎免疫反应的发展顺序。疾病早期 IFNg 水平的升高可能与心衰表现的增加有关。Th17 介导的机制可能参与了导致心肌硬化的心肌重塑过程。

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Russian Journal of Infection and Immunity

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