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Transplacental Transfer of Hepatitis B Neutralizing Antibody during Pregnancy in an Animal Model: Implications for Newborn and Maternal Health

机译:乙型肝炎中和抗体在动物模型中的经胎盘转移:对新生儿和产妇健康的影响

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摘要

Despite the success of postexposure prophylaxis (PEP) of the newborn in preventing mother-to-child transmission of hepatitis B virus), in non-US clinical trials, administering hepatitis B immune globulin (HBIG) to mothers at the end of pregnancy (in addition to passive-active PEP of the newborn) only partially improved outcomes. That is, a significant percentage of newborns became infected during their first year of life. We used a relevant animal model for human IgG transplacental transfer to study dose, time and subclass dependence of HBV neutralizing antibody (nAb) maternal, and fetal levels at the end of pregnancy. Pregnant guinea pigs received 50 or 100 IU/kg HBIGIV 2-5 days before delivery. Human total IgG, IgG subclasses, and nAb in mothers and their litters were measured .In vitro analyses of guinea pig Fc neonatal receptor binding to HBIGIV, as well as to all human IgG subclasses, were also performed. Our study showed that nAb transferred transplacentaUy from the pregnant guinea pigs to their litters; no transfer occurred during parturition. The amount of the transferred nAb was dose and time dependent. Thus, selection of an efficacious dose in the clinic is important: microdosing may be underdosing, particularly in cases of high viraemia.
机译:尽管新生儿的暴露后预防(PEP)在预防乙型肝炎病毒的母婴传播方面取得了成功),但在非美国临床试验中,在妊娠结束时向母亲服用乙型肝炎免疫球蛋白(HBIG)。除了新生儿的被动-主动式PEP)只能部分改善结局。也就是说,很大比例的新生儿在生命的第一年就被感染了。我们使用了有关人IgG经胎盘转移的相关动物模型来研究孕产期HBV中和抗体(nAb)母体的剂量,时间和亚类依赖性以及胎儿水平。怀孕的豚鼠在分娩前2-5天接受了50或100 IU / kg HBIGIV。测量母亲及其产仔中人的总IgG,IgG亚类和nAb。还进行了豚鼠Fc新生受体与HBIGIV以及所有人IgG亚类结合的体外分析。我们的研究表明,nAb将胎盘素从怀孕的豚鼠转移至其产仔。分娩过程中未发生转移。转移的nAb的量与剂量和时间有关。因此,在临床中选择有效剂量很重要:微量给药可能剂量不足,尤其是在高病毒血症的情况下。

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