Center for Global Health and Diseases, Case Western Reserve University, Cleveland, OH 44106-7286, USA.
J Infect Dis. 2010 Sep 15;202(6):899-907. doi: 10.1086/655783.
Mother-to-child-transmission (MTCT) of human immunodeficiency virus (HIV) remains a significant cause of new HIV infections in many countries. To examine whether fetal immune activation as a consequence of prenatal exposure to parasitic antigens increases the risk of MTCT, cord blood mononuclear cells (CBMCs) from Kenyan and North American newborns were examined for relative susceptibility to HIV infection in vitro. Kenyan CBMCs were 3-fold more likely to be infected with HIV than were North American CBMCs (P=.03). Kenyan CBMCs with recall responses to malaria antigens demonstrated enhanced susceptibility to HIV when compared with Kenyan CBMCs lacking recall responses to malaria (P=.03). CD4(+) T cells from malaria-sensitized newborns expressed higher levels of CD25 and human leukocyte antigen DR ex vivo, which is consistent with increased immune activation. CD4(+) T cells were the primary reservoir of infection at day 4 after virus exposure. Thus, prenatal exposure and in utero priming to malaria may increase the risk of MTCT.
母婴传播(MTCT)仍然是许多国家新发生 HIV 感染的一个重要原因。为了研究胎儿因产前暴露于寄生虫抗原而发生的免疫激活是否会增加 MTCT 的风险,我们检查了肯尼亚和北美的新生儿脐带血单核细胞(CBMC)对 HIV 感染的体外相对易感性。与北美的 CBMC 相比,肯尼亚的 CBMC 更有可能被 HIV 感染(P=.03)。与缺乏疟疾抗原回忆反应的肯尼亚 CBMC 相比,对疟疾抗原有回忆反应的肯尼亚 CBMC 对 HIV 的易感性增强(P=.03)。来自疟疾致敏新生儿的 CD4+T 细胞在体外表达更高水平的 CD25 和人类白细胞抗原 DR,这与免疫激活增加一致。CD4+T 细胞是病毒暴露后第 4 天感染的主要储存库。因此,产前暴露和宫内疟疾启动可能会增加 MTCT 的风险。