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在有或无单剂量奈韦拉平的情况下,HIV-1暴露对HIV-1血清阳性母亲所生婴儿细胞血浆活化标志物的体内影响。

In vivo effects of HIV-1 exposure in the presence and absence of single-dose nevirapine on cellular plasma activation markers of infants born to HIV-1-seropositive mothers.

作者信息

Schramm Diana B, Kuhn Louise, Gray Glenda E, Tiemessen Caroline T

机构信息

AIDS Virus Research Unit, National Institute for Communicable Diseases and Department of Virology, University of the Witwatersrand, Gauteng, South Africa.

出版信息

J Acquir Immune Defic Syndr. 2006 Aug 15;42(5):545-53. doi: 10.1097/01.qai.0000225009.30698.ce.

Abstract

Short-course antiretroviral drug regimens reduce the risk of mother-to-child transmission of HIV-1, but mechanisms affording protection of such interventions remain poorly defined. Because T-cell activation is an important factor in productive HIV-1 infection, we tested the hypothesis that single-dose nevirapine (NVP) reduces immune activation, which in turn reduces the likelihood of transmission. We compared concentrations of cord and maternal blood plasma immune activation markers, neopterin, beta2-microglobulin, and soluble l-selectin, in 2 groups of HIV-1-exposed newborns whose mothers either received NVP at the onset of labor or who only received NVP as postexposure prophylaxis within 72 hours of birth and among HIV-unexposed controls. In utero exposure of the infant to HIV-1, regardless of NVP exposure, led to demonstrable increases in immune activation markers, this being most notable in the presence of preexisting infection. Contrary to what was hypothesized, immune activation was increased by prebirth exposure to single-dose NVP, with this effect being enhanced in infants already infected at birth. Our data suggest that reductions in immune activation do not explain transmission prevention effects of single-dose NVP. Our data also suggest a biological explanation for why HIV-1-infected infants exposed perinatally to antiretroviral drugs might experience hastened disease progression, namely, in some HIV-1-infected individuals, NVP may synergize with HIV-1 to enhance an environment that favors increased HIV-1 replication.

摘要

短期抗逆转录病毒药物治疗方案可降低HIV-1母婴传播风险,但此类干预措施提供保护的机制仍不清楚。由于T细胞活化是HIV-1有效感染的一个重要因素,我们检验了单剂量奈韦拉平(NVP)可降低免疫活化,进而降低传播可能性的假设。我们比较了两组暴露于HIV-1的新生儿脐血和母血血浆中免疫活化标志物(新蝶呤、β2-微球蛋白和可溶性L-选择素)的浓度,这两组新生儿的母亲分别在分娩开始时接受NVP,或仅在出生后72小时内接受NVP作为暴露后预防,同时还比较了未暴露于HIV的对照组。无论是否暴露于NVP,婴儿在子宫内暴露于HIV-1都会导致免疫活化标志物明显增加,在已有感染的情况下最为明显。与假设相反,产前暴露于单剂量NVP会增加免疫活化,在出生时已感染的婴儿中这种效应会增强。我们的数据表明,免疫活化的降低并不能解释单剂量NVP预防传播的效果。我们的数据还为围产期暴露于抗逆转录病毒药物的HIV-1感染婴儿为何可能经历疾病进展加速提供了生物学解释,即,在一些HIV-1感染个体中,NVP可能与HIV-1协同作用,增强有利于HIV-1复制增加的环境。

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