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母体自体中和抗体在1型人类免疫缺陷病毒逃逸变异体选择性围产期传播中的作用

Role of maternal autologous neutralizing antibody in selective perinatal transmission of human immunodeficiency virus type 1 escape variants.

作者信息

Dickover Ruth, Garratty Eileen, Yusim Karina, Miller Catherine, Korber Bette, Bryson Yvonne

机构信息

Department of Pediatrics, David Geffen School of Medicine at UCLA, University of California-Los Angeles, 10833 LeConte Ave., Los Angeles, CA 90095, USA.

出版信息

J Virol. 2006 Jul;80(13):6525-33. doi: 10.1128/JVI.02658-05.

Abstract

Perinatal human immunodeficiency virus type 1 (HIV-1) transmission is characterized by acquisition of a homogeneous viral quasispecies, yet the selective factors responsible for this genetic bottleneck are unclear. We examined the role of maternal autologous neutralizing antibody (aNAB) in selective transmission of HIV-1 escape variants to infants. Maternal sera from 38 infected mothers at the time of delivery were assayed for autologous neutralizing antibody activity against maternal time-of-delivery HIV-1 isolates in vitro. Maternal sera were also tested for cross-neutralization of infected-infant-first-positive-time-point viral isolates. Heteroduplex and DNA sequence analyses were then performed to identify the initial infecting virus as a neutralization-sensitive or escape HIV-1 variant. In utero transmitters (n = 14) were significantly less likely to have aNAB to their own HIV-1 strains at delivery than nontransmitting mothers (n = 17, 14.3% versus 76.5%, P = 0.003). Cross-neutralization assays of infected-infant-first-positive-time-point HIV-1 isolates indicated that while 14/21 HIV-1-infected infant first positive time point isolates were resistant to their own mother's aNAB, no infant isolate was inherently resistant to antibody neutralization by all sera tested. Furthermore, both heteroduplex (n = 21) and phylogenetic (n = 9) analyses showed that selective perinatal transmission and/or outgrowth of maternal autologous neutralization escape HIV-1 variants occurs in utero and intrapartum. These data indicate that maternal autologous neutralizing antibody can exert powerful protective and selective effects in perinatal HIV-1 transmission and therefore has important implications for vaccine development.

摘要

围产期人类免疫缺陷病毒1型(HIV-1)传播的特征是获得同质化的病毒准种,但造成这种基因瓶颈的选择因素尚不清楚。我们研究了母体自身中和抗体(aNAB)在HIV-1逃逸变体向婴儿的选择性传播中的作用。对38名感染母亲分娩时的母体血清进行体外检测,以检测其针对母体分娩时HIV-1分离株的自身中和抗体活性。还检测了母体血清对感染婴儿首次阳性时间点病毒分离株的交叉中和作用。然后进行异源双链分析和DNA序列分析,以确定初始感染病毒是中和敏感型还是逃逸型HIV-1变体。与未传播的母亲(n = 17)相比,宫内传播者(n = 14)在分娩时对自身HIV-1毒株产生aNAB的可能性显著降低(14.3%对76.5%,P = 0.003)。对感染婴儿首次阳性时间点HIV-1分离株的交叉中和试验表明,虽然21株HIV-1感染婴儿首次阳性时间点分离株中有14株对其自身母亲的aNAB具有抗性,但没有婴儿分离株对所有检测血清的抗体中和作用具有固有抗性。此外,异源双链分析(n = 21)和系统发育分析(n = 9)均显示,母体自身中和逃逸HIV-1变体的选择性围产期传播和/或生长发生在子宫内和分娩时。这些数据表明,母体自身中和抗体在围产期HIV-1传播中可发挥强大的保护和选择作用,因此对疫苗开发具有重要意义。

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