E. V. Saidakova, L. Korolevskaya, V. V. Vlasova, N. Shmagel, K. Shmagel
{"title":"艾滋病毒/艾滋病合并感染者中对抗逆病毒疗法无免疫反应的 CD4⁺ 和 CD8⁺ T 细胞衰竭的标志物","authors":"E. V. Saidakova, L. Korolevskaya, V. V. Vlasova, N. Shmagel, K. Shmagel","doi":"10.15789/2220-7619-mic-16641","DOIUrl":null,"url":null,"abstract":"Coinfection with human immunodeficiency virus (HIV) and hepatitis C virus (HCV) is a risk factor for immunological non-response to antiretroviral therapy. In cases of immunological non-response, HIV viral load suppression occurs without an increase in CD4⁺ T-cell counts, heightening the risk of morbidity and mortality in infected individuals. T-cell exhaustion may hinder their regeneration in immunological non-responders. This study aimed to identify markers of CD4⁺ and CD8⁺ T-cell exhaustion in HIV/HCV coinfected immunological non-responders. The study examined three clinical groups: 1) HIV/HCV coinfected immunological non-responders (CD4⁺ T-cells 350/µl blood; n = 9), 2) HIV/HCV coinfected individuals with a standard response to therapy (CD4⁺ T-cells 500/µl blood; n = 9), and 3) relatively healthy volunteers without HIV and HCV infections (n = 9). Ex vivo, the number of CD4⁺ and CD8⁺ T-cells expressing the inhibitory receptor PD-1 was determined using multi-color flow cytometry. In the 7-day in vitro experiment, cell cultures were stimulated with phytohemagglutinin. The number of dying proliferated CD4⁺ and CD8⁺ T-cells (CFSElowZombieUV+) was determined using multi-color flow cytometry. The amount of interleukin-2 in the culture supernatants was measured using an enzyme-linked immunosorbent assay. It was found that in HIV/HCV coinfected immunological non-responders, there was a higher number of CD4⁺ and CD8⁺ T-cells expressing PD-1, a phenotypic marker of exhaustion, compared to the other two groups. Furthermore, the frequency of dying dividing T-cells was higher in immunological non-responders, with an increase in CD4⁺ T-cells but not CD8⁺ T-lymphocytes. Similarly, a decrease in interleukin-2 production was found in stimulated T-cells of HIV/HCV coinfected immunological non-responders in the CD4⁺ T-cell pool, but not in CD8⁺ T-lymphocytes. Thus, in HIV/HCV coinfected immunological non-responders, CD4⁺ T-cells appear exhausted both phenotypically and functionally. While CD8⁺ T-cells express inhibitory receptors, they do not show functional impairments. It appears that the specialized therapy for HIV/HCV coinfected immunological non-responders should aim to improve CD4⁺ T-cell function.","PeriodicalId":21412,"journal":{"name":"Russian Journal of Infection and Immunity","volume":"4 12","pages":""},"PeriodicalIF":0.0000,"publicationDate":"2024-07-28","publicationTypes":"Journal Article","fieldsOfStudy":null,"isOpenAccess":false,"openAccessPdf":"","citationCount":"0","resultStr":"{\"title\":\"Markers of CD4⁺ AND CD8⁺ T-cell exhaustion in hiv/hcv coinfected immunological non-responders to antiretroviral therapy\",\"authors\":\"E. V. Saidakova, L. Korolevskaya, V. V. Vlasova, N. Shmagel, K. Shmagel\",\"doi\":\"10.15789/2220-7619-mic-16641\",\"DOIUrl\":null,\"url\":null,\"abstract\":\"Coinfection with human immunodeficiency virus (HIV) and hepatitis C virus (HCV) is a risk factor for immunological non-response to antiretroviral therapy. In cases of immunological non-response, HIV viral load suppression occurs without an increase in CD4⁺ T-cell counts, heightening the risk of morbidity and mortality in infected individuals. T-cell exhaustion may hinder their regeneration in immunological non-responders. This study aimed to identify markers of CD4⁺ and CD8⁺ T-cell exhaustion in HIV/HCV coinfected immunological non-responders. The study examined three clinical groups: 1) HIV/HCV coinfected immunological non-responders (CD4⁺ T-cells 350/µl blood; n = 9), 2) HIV/HCV coinfected individuals with a standard response to therapy (CD4⁺ T-cells 500/µl blood; n = 9), and 3) relatively healthy volunteers without HIV and HCV infections (n = 9). Ex vivo, the number of CD4⁺ and CD8⁺ T-cells expressing the inhibitory receptor PD-1 was determined using multi-color flow cytometry. In the 7-day in vitro experiment, cell cultures were stimulated with phytohemagglutinin. The number of dying proliferated CD4⁺ and CD8⁺ T-cells (CFSElowZombieUV+) was determined using multi-color flow cytometry. The amount of interleukin-2 in the culture supernatants was measured using an enzyme-linked immunosorbent assay. It was found that in HIV/HCV coinfected immunological non-responders, there was a higher number of CD4⁺ and CD8⁺ T-cells expressing PD-1, a phenotypic marker of exhaustion, compared to the other two groups. Furthermore, the frequency of dying dividing T-cells was higher in immunological non-responders, with an increase in CD4⁺ T-cells but not CD8⁺ T-lymphocytes. Similarly, a decrease in interleukin-2 production was found in stimulated T-cells of HIV/HCV coinfected immunological non-responders in the CD4⁺ T-cell pool, but not in CD8⁺ T-lymphocytes. Thus, in HIV/HCV coinfected immunological non-responders, CD4⁺ T-cells appear exhausted both phenotypically and functionally. While CD8⁺ T-cells express inhibitory receptors, they do not show functional impairments. 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引用次数: 0
摘要
人类免疫缺陷病毒(HIV)和丙型肝炎病毒(HCV)合并感染是导致抗逆转录病毒疗法免疫无反应的一个风险因素。在免疫无应答的情况下,HIV 病毒载量会被抑制,而 CD4⁺ T 细胞数量不会增加,从而增加了感染者发病和死亡的风险。T细胞衰竭可能会阻碍免疫无反应者T细胞的再生。本研究旨在确定HIV/HCV双重感染免疫无应答者CD4⁺和CD8⁺T细胞衰竭的标志物。研究考察了三个临床组:1)HIV/HCV 合并感染的免疫无反应者(CD4⁺ T 细胞 350/µl 血液;n = 9);2)对治疗有标准反应的 HIV/HCV 合并感染者(CD4⁺ T 细胞 500/µl 血液;n = 9);3)未感染 HIV 和 HCV 的相对健康的志愿者(n = 9)。体外实验中,使用多色流式细胞术测定了表达抑制性受体 PD-1 的 CD4⁺ 和 CD8⁺ T 细胞的数量。在为期 7 天的体外实验中,细胞培养物受到植物血凝素的刺激。使用多色流式细胞术测定了死亡增殖的 CD4⁺ 和 CD8⁺ T 细胞(CFSElowZombieUV+)的数量。培养上清液中的白细胞介素-2 含量采用酶联免疫吸附测定法进行测定。研究发现,与其他两组相比,HIV/HCV 合并感染的免疫无应答者中表达 PD-1 的 CD4⁺ 和 CD8⁺ T 细胞数量较多,而 PD-1 是衰竭的表型标记。此外,免疫无应答者中濒死分裂 T 细胞的频率更高,CD4⁺ T 细胞增加,但 CD8⁺ T 淋巴细胞没有增加。同样,HIV/HCV 共感染免疫无反应者的 CD4⁺ T 细胞池中,受刺激的 T 细胞中白细胞介素-2 的产生量减少,但 CD8⁺ T 淋巴细胞中的白细胞介素-2 的产生量没有减少。因此,在艾滋病毒/HCV 共同感染的免疫无反应者中,CD4⁺ T 细胞在表型和功能上都已耗竭。虽然 CD8⁺ T 细胞表达抑制性受体,但它们并没有表现出功能障碍。由此看来,针对艾滋病毒/丙型肝炎病毒双重感染免疫无反应者的专门疗法应以改善 CD4⁺ T 细胞功能为目标。
Markers of CD4⁺ AND CD8⁺ T-cell exhaustion in hiv/hcv coinfected immunological non-responders to antiretroviral therapy
Coinfection with human immunodeficiency virus (HIV) and hepatitis C virus (HCV) is a risk factor for immunological non-response to antiretroviral therapy. In cases of immunological non-response, HIV viral load suppression occurs without an increase in CD4⁺ T-cell counts, heightening the risk of morbidity and mortality in infected individuals. T-cell exhaustion may hinder their regeneration in immunological non-responders. This study aimed to identify markers of CD4⁺ and CD8⁺ T-cell exhaustion in HIV/HCV coinfected immunological non-responders. The study examined three clinical groups: 1) HIV/HCV coinfected immunological non-responders (CD4⁺ T-cells 350/µl blood; n = 9), 2) HIV/HCV coinfected individuals with a standard response to therapy (CD4⁺ T-cells 500/µl blood; n = 9), and 3) relatively healthy volunteers without HIV and HCV infections (n = 9). Ex vivo, the number of CD4⁺ and CD8⁺ T-cells expressing the inhibitory receptor PD-1 was determined using multi-color flow cytometry. In the 7-day in vitro experiment, cell cultures were stimulated with phytohemagglutinin. The number of dying proliferated CD4⁺ and CD8⁺ T-cells (CFSElowZombieUV+) was determined using multi-color flow cytometry. The amount of interleukin-2 in the culture supernatants was measured using an enzyme-linked immunosorbent assay. It was found that in HIV/HCV coinfected immunological non-responders, there was a higher number of CD4⁺ and CD8⁺ T-cells expressing PD-1, a phenotypic marker of exhaustion, compared to the other two groups. Furthermore, the frequency of dying dividing T-cells was higher in immunological non-responders, with an increase in CD4⁺ T-cells but not CD8⁺ T-lymphocytes. Similarly, a decrease in interleukin-2 production was found in stimulated T-cells of HIV/HCV coinfected immunological non-responders in the CD4⁺ T-cell pool, but not in CD8⁺ T-lymphocytes. Thus, in HIV/HCV coinfected immunological non-responders, CD4⁺ T-cells appear exhausted both phenotypically and functionally. While CD8⁺ T-cells express inhibitory receptors, they do not show functional impairments. It appears that the specialized therapy for HIV/HCV coinfected immunological non-responders should aim to improve CD4⁺ T-cell function.
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