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妊娠对 HIV-1 特异性颗粒酶 B 反应和中央记忆 CD4 T 细胞的影响。

Pregnancy Gestation Impacts on HIV-1-Specific Granzyme B Response and Central Memory CD4 T Cells.

机构信息

Imperial College London, London, United Kingdom.

Chelsea and Westminster Hospital, London, United Kingdom.

出版信息

Front Immunol. 2020 Feb 11;11:153. doi: 10.3389/fimmu.2020.00153. eCollection 2020.

Abstract

Pregnancy induces alterations in peripheral T-cell populations with both changes in subset frequencies and anti-viral responses found to alter with gestation. In HIV-1 positive women anti-HIV-1 responses are associated with transmission risk, however detailed investigation into both HIV-1-specific memory responses associated with HIV-1 control and T-cell subset changes during pregnancy have not been undertaken. In this study we aimed to define pregnancy and gestation related changes to HIV-1-specific responses and T-cell phenotype in ART treated HIV-1 positive pregnant women. Eleven non-pregnant and 24 pregnant HIV-1 positive women were recruited, peripheral blood samples taken, fresh cells isolated, and compared using ELISpot assays and flow cytometry analysis. Clinical data were collected as part of standard care, and non-parametric statistics used. Alterations in induced IFNγ, IL-2, IL-10, and granzyme B secretion by peripheral blood mononuclear cells in response to HIV-1 Gag and Nef peptide pools and changes in T-cell subsets between pregnant and non-pregnant women were assessed, with data correlated with participant clinical parameters and longitudinal analysis performed. Cross-sectional comparison identified decreased IL-10 Nef response in HIV-1 positive pregnant women compared to non-pregnant, while correlations exhibited reversed Gag and Nef cytokine and protease response associations between groups. Longitudinal analysis of pregnant participants demonstrated transient increases in Gag granzyme B response and in the central memory CD4 T-cell subset frequency during their second trimester, with a decrease in CD4 effector memory T cells from their second to third trimester. Gag and Nef HIV-1-specific responses diverge with pregnancy time-point, coinciding with relevant T-cell phenotype, and gestation associated immunological adaptations. Decreased IL-10 Nef and both increased granzyme B Gag response and central memory CD4 T cells implies that amplified antigen production is occurring, which suggests a period of compromised HIV-1 control in pregnancy.

摘要

妊娠可引起外周 T 细胞群体的改变,包括亚群频率的变化和抗病毒反应的变化,这些变化随着妊娠而改变。在 HIV-1 阳性妇女中,抗 HIV-1 反应与传播风险相关,然而,尚未对与 HIV-1 控制相关的 HIV-1 特异性记忆反应以及妊娠期间 T 细胞亚群变化进行详细研究。在这项研究中,我们旨在确定接受 ART 治疗的 HIV-1 阳性孕妇中与 HIV-1 特异性反应和 T 细胞表型相关的妊娠和妊娠相关变化。招募了 11 名非妊娠和 24 名妊娠 HIV-1 阳性妇女,采集外周血样本,分离新鲜细胞,并使用 ELISpot 测定和流式细胞术分析进行比较。临床数据作为标准护理的一部分收集,并使用非参数统计。评估外周血单核细胞对 HIV-1 Gag 和 Nef 肽库诱导 IFNγ、IL-2、IL-10 和颗粒酶 B 分泌的变化,以及妊娠和非妊娠妇女之间 T 细胞亚群的变化,并将数据与参与者的临床参数相关联,并进行纵向分析。横断面比较发现,与非妊娠妇女相比,HIV-1 阳性妊娠妇女的 HIV-1 Nef 反应中 IL-10 减少,而相关性分析显示两组之间 Gag 和 Nef 细胞因子和蛋白酶反应的相关性发生逆转。对妊娠参与者的纵向分析表明,在妊娠中期,Gag 颗粒酶 B 反应和中央记忆 CD4 T 细胞亚群频率短暂增加,而从妊娠中期到妊娠晚期,CD4 效应记忆 T 细胞减少。Gag 和 Nef HIV-1 特异性反应随着妊娠时间点的不同而不同,与相关的 T 细胞表型和妊娠相关的免疫适应一致。Nef 反应中 IL-10 的减少以及 Gag 反应中颗粒酶 B 和中央记忆 CD4 T 细胞的增加意味着扩增的抗原产生正在发生,这表明妊娠期间 HIV-1 控制受损。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/7a63/7027986/2f19f367f7c4/fimmu-11-00153-g0001.jpg

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