Influence of HIV-infection on clinical course and a frequency of antibody response to the new coronavirus infection

A. Danilov, T. L. Abramyan, V. I. Eremin, Natalya A. Philippova
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Abstract

Background. The clinical course of COVID-19 infection can be significantly affected by severe immunosuppression, viral load, concomitant diseases and conditions not related to HIV, the absence of antiretroviral therapy. It is potentially important to assess the state of post-ovoid immunity for the provision of medical care to HIV-infected patients with COVID-19. Aim: to assess the impact of HIV infection on the clinical course of a new coronavirus infection, the severity of the disease and its outcomes, and immune response. Materials and methods. Medical records of 35,328 patients who underwent COVID-19 in 2020 were analyzed, including 46 cases of SARS-CoV-2 infection in HIV-infected individuals. To determine specific antibodies to SARS-CoV-2, 281 blood samples were examined by ELISA. The clinical course of COVID-19 in HIV-infected patients, as well as the production of IgG to SARS-CoV-2, depending on the level of CD4 and viral load, were assessed. Results. In 76% of co-infected patients, there were signs of progression of HIV infection, opportunistic infections and concomitant diseases. 52.2% of the analyzed group were users of psychoactive substances. Among patients co-infected with HIV and COVID-19, men predominated in the age groups over 30 years old, while among the HIV-negative population, women in the age groups over 18 years old predominated. The proportion of severe forms of COVID-19 in HIV-infected people (47.8%) exceeds that in the group of patients without immunodeficiency (12.3%). The mortality rate from COVID-19 among HIV-infected people was more than 7 times higher than that of the HIV-negative population of the region (t=1.81; p=0.01). Among the examined 72 HIV-infected patients, IgG antibodies to SARS-CoV-2 were detected in 20 patients, of which 4 (28.5%) with confirmed HIV/SARS-CoV-2 co-infection and 16 people (27.5%) without medical confirmation. HIV-infected patients with severe immunodeficiency did not develop a humoral immune response to COVID-19 infection, and in 25% the immune response lasted less than 3 months. Conclusions. HIV-infected patients are at greater risk of developing a severe course of coronavirus infection. The presence of deep immunodeficiency and high viral load in patients without antiretroviral therapy significantly reduces tension and shortens the development and duration of post-COVID immunity.
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hiv感染对新型冠状病毒感染临床病程及抗体应答频率的影响
背景。严重的免疫抑制、病毒载量、与艾滋病毒无关的伴随疾病和病症以及缺乏抗逆转录病毒治疗可显著影响COVID-19感染的临床病程。评估卵泡后免疫状态对于向感染艾滋病毒的COVID-19患者提供医疗服务具有潜在的重要意义。目的:评估HIV感染对新型冠状病毒感染的临床病程、病情严重程度及其结局、免疫反应的影响。材料和方法。分析了2020年35328例新冠肺炎患者的医疗记录,其中包括46例hiv感染者的SARS-CoV-2感染病例。为确定SARS-CoV-2特异性抗体,对281份血样进行了ELISA检测。评估了hiv感染患者的COVID-19临床病程,以及根据CD4水平和病毒载量产生的针对SARS-CoV-2的IgG。结果。在76%的合并感染患者中,有艾滋病毒感染进展、机会性感染和伴随疾病的迹象。52.2%的分析组为精神活性物质使用者。在合并感染艾滋病毒和COVID-19的患者中,30岁以上年龄组的男性居多,而在艾滋病毒阴性人群中,18岁以上年龄组的女性居多。艾滋病毒感染者中严重形式COVID-19的比例(47.8%)超过无免疫缺陷患者组(12.3%)。该地区hiv感染者的COVID-19死亡率是hiv阴性人群的7倍以上(t=1.81;p = 0.01)。在72例HIV感染者中,20例患者检测到SARS-CoV-2 IgG抗体,其中4例(28.5%)确诊为HIV/SARS-CoV-2合并感染,16例(27.5%)无医学证实。严重免疫缺陷的hiv感染患者对COVID-19感染没有产生体液免疫反应,25%的免疫反应持续时间不到3个月。结论。感染艾滋病毒的患者发生严重冠状病毒感染的风险更大。未接受抗逆转录病毒治疗的患者存在深度免疫缺陷和高病毒载量,可显著降低紧张感,缩短covid后免疫的发展和持续时间。
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