Department of Medicine, Boston University School of Medicine, Boston, Massachusetts, USA.
Department of Biostatistics, Boston University School of Public Health, Boston, Massachusetts, USA.
mBio. 2017 Oct 24;8(5):e01373-17. doi: 10.1128/mBio.01373-17.
A significant number of infants acquire HIV-1 through their infected mother's breast milk, primarily due to limited access to antiretrovirals. Passive immunization with neutralizing antibodies (nAbs) may prevent this transmission. Previous studies, however, have generated conflicting results about the ability of nAbs to halt mother-to-child transmission (MTCT) and their impact on infant outcomes. This study compared plasma neutralizing activity in exposed infants and the infected mothers ( 63) against heterologous HIV-1 variants and the quasispecies present in the mother. HIV-exposed uninfected infants (HEU) ( 42), compared to those that eventually acquired infection ( 21), did not possess higher nAb responses against heterologous envelopes ( = 0.46) or their mothers' variants ( = 0.45). Transmitting compared to nontransmitting mothers, however, had significantly higher plasma neutralizing activity against heterologous envelopes ( = 0.03), although these two groups did not have significant differences in their ability to neutralize autologous strains ( = 0.39). Furthermore, infants born to mothers with greater neutralizing breadth and potency were significantly more likely to have a serious adverse event ( = 0.03). These results imply that preexisting anti-HIV-1 neutralizing activity does not prevent breast milk transmission. Additionally, high maternal neutralizing breadth and potency may adversely influence both the frequency of breast milk transmission and subsequent infant morbidity. Passive immunization trials are under way to understand if preexisting antibodies can decrease mother-to-child HIV-1 transmission and improve infant outcomes. We examined the influence of preexisting maternal and infant neutralizing activity on transmission and infant morbidity in a breastfeeding mother-infant cohort. Neutralization was examined against both the exposure strains circulating in the infected mothers and a standardized reference panel previously used to estimate breadth. HIV-exposed uninfected infants did not possess a broader and more potent response against both the exposure and heterologous strains compared to infants that acquired infection. Transmitting, compared to nontransmitting, mothers had significantly higher neutralization breadth and potency but similar responses against autologous variants. Infants born to mothers with higher neutralization responses were more likely to have a serious adverse event. Our results suggest that preexisting antibodies do not protect against breast milk HIV-1 acquisition and may have negative consequences for the baby.
大量婴儿通过受感染母亲的母乳感染 HIV-1,主要是因为获得抗逆转录病毒药物的机会有限。使用中和抗体(nAbs)进行被动免疫可能会阻止这种传播。然而,先前的研究对抗 nAbs 阻止母婴传播(MTCT)的能力及其对婴儿结局的影响产生了相互矛盾的结果。本研究比较了暴露于 HIV 的婴儿和感染母亲(63 例)的血浆中和活性,以对抗异源 HIV-1 变体和母亲体内的准种。与最终感染的婴儿(21 例)相比,未感染的 HIV 暴露婴儿(HEU)(42 例)对异源包膜的 nAb 反应并没有更高(=0.46)或对其母亲变体的反应更高(=0.45)。与非传播母亲相比,传播母亲的血浆对异源包膜的中和活性显著更高(=0.03),尽管这两组在中和自身株的能力上没有显著差异(=0.39)。此外,来自具有更高中和广度和效力的母亲的婴儿更有可能发生严重不良事件(=0.03)。这些结果表明,预先存在的抗 HIV-1 中和活性并不能阻止母乳传播。此外,高母体中和广度和效力可能会对母乳传播的频率和随后婴儿发病率产生不利影响。正在进行被动免疫试验,以了解预先存在的抗体是否可以降低母婴 HIV-1 传播并改善婴儿结局。我们在一个母乳喂养母婴队列中研究了预先存在的母婴中和活性对传播和婴儿发病率的影响。中和活性针对感染母亲循环的暴露株和以前用于估计广度的标准化参考面板进行了检测。与感染的婴儿相比,未感染的 HIV 暴露婴儿对暴露株和异源株的反应既不更广泛也不更有效。与非传播母亲相比,传播母亲的中和广度和效力显著更高,但对自身变体的反应相似。来自中和反应较高的母亲的婴儿更有可能发生严重不良事件。我们的结果表明,预先存在的抗体不能保护婴儿免受母乳中 HIV-1 的感染,并且可能对婴儿产生负面影响。
