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在肯尼亚新生儿中,妊娠期间的 HIV、巨细胞病毒和疟疾感染会导致炎症和记忆 B 细胞亚群的变化。

HIV, Cytomegalovirus, and Malaria Infections during Pregnancy Lead to Inflammation and Shifts in Memory B Cell Subsets in Kenyan Neonates.

机构信息

Center for Global Health and Diseases, Case Western Reserve University, Cleveland, OH 44106.

Department of Pediatrics, Rainbow Babies and Children's Hospital, Case Western Reserve University, Cleveland, OH 44106; and.

出版信息

J Immunol. 2019 Mar 1;202(5):1465-1478. doi: 10.4049/jimmunol.1801024. Epub 2019 Jan 23.

Abstract

Infections during pregnancy can expose the fetus to microbial Ags, leading to inflammation that affects B cell development. Prenatal fetal immune priming may have an important role in infant acquisition of pathogen-specific immunity. We examined plasma proinflammatory biomarkers, the proportions of various B cell subsets, and fetal priming to tetanus vaccination in cord blood from human United States and Kenyan neonates. United States neonates had no identified prenatal infectious exposures, whereas Kenyan neonates examined had congenital CMV or mothers with prenatal HIV or or no identified infectious exposures. Kenyan neonates had higher levels of IP-10, TNF-α, CRP, sCD14, and BAFF than United States neonates. Among the Kenyan groups, neonates with prenatal infections/infectious exposures had higher levels of cord blood IFN-γ, IL-7, sTNFR1, and sTNFR2 compared with neonates with no infectious exposures. Kenyan neonates had greater proportions of activated memory B cells (MBC) compared with United States neonates. Among the Kenyan groups, HIV-exposed neonates had greater proportions of atypical MBC compared with the other groups. Although HIV-exposed neonates had altered MBC subset distributions, detection of tetanus-specific MBC from cord blood, indicative of fetal priming with tetanus vaccine given to pregnant women, was comparable in HIV-exposed and non-HIV-exposed neonates. These results indicate that the presence of infections during pregnancy induces fetal immune activation with inflammation and increased activated MBC frequencies in neonates. The immunologic significance and long-term health consequences of these differences warrant further investigation.

摘要

妊娠期间的感染可能使胎儿暴露于微生物抗原,导致影响 B 细胞发育的炎症。产前胎儿免疫启动可能在婴儿获得针对病原体的特异性免疫方面发挥重要作用。我们检查了来自美国和肯尼亚新生儿脐带血中的促炎生物标志物、各种 B 细胞亚群的比例以及破伤风疫苗的胎儿免疫启动情况。美国新生儿没有明确的产前感染暴露,而肯尼亚新生儿中检查出先天性 CMV 或母亲有产前 HIV 或其他未确定的感染暴露。肯尼亚新生儿的 IP-10、TNF-α、CRP、sCD14 和 BAFF 水平高于美国新生儿。在肯尼亚各组中,与无感染暴露的新生儿相比,有产前感染/感染暴露的新生儿的脐带血 IFN-γ、IL-7、sTNFR1 和 sTNFR2 水平更高。与美国新生儿相比,肯尼亚新生儿的活化记忆 B 细胞(MBC)比例更高。在肯尼亚各组中,与其他组相比,HIV 暴露的新生儿具有更高比例的非典型 MBC。尽管 HIV 暴露的新生儿具有改变的 MBC 亚群分布,但从脐带血中检测到破伤风特异性 MBC,表明对孕妇给予破伤风疫苗的胎儿免疫启动,在 HIV 暴露和非 HIV 暴露的新生儿中是相当的。这些结果表明,妊娠期间存在感染会诱导胎儿免疫激活、炎症和增加新生儿中活化的 MBC 频率。这些差异的免疫意义和长期健康后果值得进一步研究。

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