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孕期免疫激活:对感染和未感染HIV的女性淋巴细胞表型及血清激活分子的系列检测

Immunologic activation during pregnancy: serial measurement of lymphocyte phenotype and serum activation molecules in HIV-infected and uninfected women.

作者信息

Mikyas Y, Aziz N, Harawa N, Gorre M, Neagos N, Nogueira M, Wafer D, Dillon M, Boyer P J, Bryson Y J, Plaeger S

机构信息

Department of Pediatrics, Marion Davies Children's Center, UCLA School of Medicine 90095-1752, USA.

出版信息

J Reprod Immunol. 1997 Jun;33(2):157-70. doi: 10.1016/s0165-0378(97)00018-1.

Abstract

Immunologic alterations occur during pregnancy, but the effect of pregnancy on HIV infection is controversial. We characterized some of the immunologic alterations with potential to influence HIV disease in 99 infected and 46 uninfected women during pregnancy and up to 6 months post-partum. Immunophenotyping to quantitate the major lymphocyte subsets and determine expression of activation and adhesion molecules on T cells was performed using 3-color staining and laser flow cytometry. Serum neopterin, beta 2-microglobulin, and tumor necrosis factor-alpha (TNF alpha) were quantitated using commercial immunoassays. HIV + pregnant women were compared to uninfected pregnant subjects and to reference ranges established on healthy, HIV-seronegative non-pregnant female controls. Both CD4 and CD8 T cell subsets were increased in HIV-negative pregnant women compared to non-pregnant controls. In HIV-infected pregnant women, CD4 T cells were low and CD8 cells were elevated compared to HIV-negative pregnant and non-pregnant women. Levels of subsets were stable during pregnancy and postpartum in both groups of women. Evidence of peripheral immune activation was found during the later stages of pregnancy. Increases in HLA-DR and CD38 activation antigens on CD8 cells, serum neopterin and beta-2-microglobulin were seen during pregnancy in HIV-negative women. These correlates of immune activation were increased in HIV-infected pregnant women and increased further during pregnancy, paralleling changes seen in uninfected pregnant women. These immunologic alterations may directly or indirectly enhance viral replication, impacting the long-term course of HIV disease.

摘要

孕期会发生免疫改变,但孕期对HIV感染的影响存在争议。我们对99名感染HIV的孕妇和46名未感染HIV的孕妇在孕期及产后6个月内的一些可能影响HIV疾病的免疫改变进行了特征分析。使用三色染色和激光流式细胞术进行免疫表型分析,以定量主要淋巴细胞亚群并确定T细胞上激活分子和黏附分子的表达。使用商业免疫测定法定量血清新蝶呤、β2-微球蛋白和肿瘤坏死因子-α(TNFα)。将感染HIV的孕妇与未感染的孕妇以及在健康、HIV血清阴性的非孕妇对照中建立的参考范围进行比较。与未怀孕的对照组相比,HIV阴性孕妇的CD4和CD8 T细胞亚群均增加。与HIV阴性孕妇和未怀孕女性相比,感染HIV的孕妇中CD4 T细胞较低而CD8细胞升高。两组女性在孕期和产后亚群水平均稳定。在孕期后期发现了外周免疫激活的证据。HIV阴性女性在孕期可见CD8细胞上HLA-DR和CD38激活抗原增加、血清新蝶呤和β2-微球蛋白增加。这些免疫激活的相关指标在感染HIV的孕妇中增加,且在孕期进一步升高,与未感染孕妇中观察到的变化相似。这些免疫改变可能直接或间接增强病毒复制,影响HIV疾病的长期病程。

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