rs11385942和rs657152变异与接受法非拉韦和雷米替韦治疗的患者的COVID-19严重程度和预后无关

S. Abdullaev, N. Denisenko, I. Temirbulatov, A. Kachanova, S. N. Tuchkova, E. Mikhaylenko, A. V. Kryukov, T. T. Valiev, K. Mirzaev, D. Sychev
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摘要

背景。越来越多的科学文献证明,感染 SARS-CoV-2 的易感性可能存在差异。COVID-19 症状的严重程度可从无症状到严重呼吸衰竭,需要长时间人工通气。造成这一系列临床表现的根本原因仍不清楚。确定可能导致临床症状变化的风险因素对于确定高风险的易感人群非常重要。这将有助于改进预防措施、减少住院人数并降低该疾病的死亡率。此前,已发现 COVID-19 的严重程度与遗传标记 rs11385942 G>GA 和 rs657152 A>C 之间存在关联。评估携带多态性标记 rs11385942 G>GA 和 rs657152 A>C 对接受特定治疗的患者 COVID-19 严重程度的影响。材料和方法。研究共纳入 240 名冠状病毒感染住院患者。所有患者均接受了法非吡韦或雷米替韦治疗。所有患者的rs11385942 G>GA和rs657152 A>C变异均已确定。研究比较了所调查标记物等位基因变异携带者的住院时间、患者转入重症监护室(ICU)的频率以及临床结果(康复或死亡)的频率。结果显示,rs11385942 G>GA和rs657152 A>C等位基因的携带与患者的住院时间、转入重症监护室的频率以及患者的预后之间没有明显的关联。rs11385942 G>GA和rs657152 A>C变异株的携带不会影响COVID-19患者临床结局的严重程度或类型。
本文章由计算机程序翻译,如有差异,请以英文原文为准。
The rs11385942 and rs657152 variants are not associated with COVID-19 severity and outcomes in patients treated with favipiravir and remdesivir
Background. There is a mounting evidence in the scientific literature that susceptibility to SARS-CoV-2 infection could vary. The severity of COVID-19 symptoms can  range from asymptomatic to severe respiratory failure, requiring prolonged artificial ventilation. The underlying causes of this range of clinical manifestations remain unclear. Identification of the risk factors that may cause this variation in clinical symptoms is important for identifying the most susceptible populations at highest risk. This should help improve prevention measures, reduce hospitalizations, and decrease the mortality rate of the disease. Previously, an association has been found between the severity of COVID-19 and the genetic markers rs11385942 G>GA and rs657152 A>C.The aim. To assess the impact of carrying polymorphic markers rs11385942 G>GA and rs657152 A>C on the severity of COVID-19 in patients undergoing specific therapy. Materials and methods. A total of 240 patients hospitalized with a coronavirus infection were included in the study. All patients received therapy with favipiravir or remdesivir. The presence of the rs11385942 G>GA and rs657152 A>C variants was determined in all patients. The study compared the length of hospital stays, frequency of patient transfers to the intensive care unit (ICU), and frequency of clinical outcomes (recovery or death) among carriers of allelic variants of the markers under investigation.Results. There were no significant associations between the carriage of variants rs11385942 G>GA and rs657152 A>C and the duration of patients’ hospitalization, frequency of patient transfers to the ICU, and patient outcomes.Conclusion. The carriage of rs11385942 G>GA and rs657152 A>C variants did not affect the severity or type of clinical outcomes in patients with COVID-19.
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