[Development and preservation of specific T-cell immunity after COVID-19 or vaccination against this infection].

Q3 Medicine
M S Blyakher, I M Fedorova, E A Tulskaya, I V Kapustin, S I Koteleva, Z K Ramazanova, E E Odintsov, S V Sandalova, L I Novikova, A V Aleshkin, S S Bochkareva
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引用次数: 0

Abstract

Aim evaluation of specific T-cell immunity against SARS-CoV-2 in primary and secondary response to virus antigens by screening method.

Materials and methods: Patients were tested 11.5 months after COVID-19 and 610 months before and after vaccination. Healthy volunteers were screened before, 26 times during the vaccination course, and 68 months after revaccination with the Sputnik V vaccine. IgG and IgM antibodies to SARS-CoV-2 were detected by ELISA using commercially available kits (Vector-Best, Russia). Antigenic (AG) activation of T cells in the fraction of bloods mononuclear cells was assessed by IFN- production after AG stimulation in the wells of plates from ELISA kits intended for detection of antibodies against SARS-CoV-2. Data were processed by MS Excel and Statistica 10.0 software.

Results: AG-specific T cells were detected in 88.5% of vaccinated healthy volunteers, half of whom were found to have T cells appearing earlier than antibodies to AG. After 6-8 months, the level of AG activation decreases. Following the revaccination, the level of AG activation of memory T cells in vitro increases within six months in 76.9100.0% of vaccinated subjects. On the contrary, after COVID-19, 86.7% of individuals had in their blood the AG-specific T cells with high activity at the time of vaccination. The activity of T cells recognizing the RBD domain of the SARS-CoV-2 S protein and the proportion of individuals who had these cells in their blood increased after the vaccination of reconvalescents.

Conclusion: T-cell immunity against SARS-CoV-2 antigens has been shown to persist for 6 months after illness. In vaccinated individuals without history of COVID-19, such duration of the preservation of AG-specific T cells in blood was only achieved after the revaccination.

[在COVID-19或针对这种感染的疫苗接种后特异性t细胞免疫的发展和保存]。
目的用筛选法评价t细胞对SARS-CoV-2病毒抗原的初次和二次应答特异性免疫。材料与方法:患者在COVID-19后11.5个月和接种疫苗前后610个月进行检测。健康志愿者在接种前、接种过程中和再次接种Sputnik V疫苗68个月后分别接受了26次筛查。采用市售试剂盒(Vector-Best, Russia),采用ELISA检测SARS-CoV-2 IgG和IgM抗体。利用检测SARS-CoV-2抗体的ELISA试剂盒,在板孔中刺激抗原(AG)后产生IFN,评估T细胞在血液单个核细胞部分中的抗原活化。数据采用MS Excel和Statistica 10.0软件处理。结果:接种疫苗的健康志愿者中有88.5%检测到AG特异性T细胞,其中一半的人发现T细胞早于AG抗体出现。6 ~ 8个月后,AG活化水平下降。再次接种后,76.9100.0%的接种者体外记忆T细胞AG激活水平在6个月内升高。相反,在COVID-19之后,86.7%的个体在接种疫苗时血液中具有高活性的ag特异性T细胞。在康复者接种疫苗后,识别sars - cov - 2s蛋白RBD结构域的T细胞活性和血液中含有这些细胞的个体比例增加。结论:对SARS-CoV-2抗原的t细胞免疫已被证明在发病后持续6个月。在没有COVID-19病史的接种过疫苗的个体中,只有在重新接种疫苗后才能实现血液中ag特异性T细胞的这种保存时间。
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来源期刊
Voprosy virusologii
Voprosy virusologii Medicine-Infectious Diseases
CiteScore
2.00
自引率
0.00%
发文量
48
期刊介绍: The journal deals with advances in virology in Russia and abroad. It publishes papers dealing with investigations of viral diseases of man, animals and plants, the results of experimental research on different problems of general and special virology. The journal publishes materials are which promote introduction into practice of the achievements of the virological science in the eradication and incidence reduction of infectious diseases, as well as their diagnosis, treatment and prevention. The reader will find a description of new methods of investigation, new apparatus and devices.
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