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赞比亚母婴对腺病毒中和反应的纵向定量研究:HIV-1 感染及其治疗的影响。

Longitudinal quantification of adenovirus neutralizing responses in Zambian mother-infant pairs: Impact of HIV-1 infection and its treatment.

机构信息

Nebraska Center for Virology and School of Biological Sciences, University of Nebraska, Lincoln, Nebraska, USA.

Nebraska Center for Virology and School of Biological Sciences, University of Nebraska, Lincoln, Nebraska, USA.

出版信息

Vaccine. 2019 Aug 23;37(36):5177-5184. doi: 10.1016/j.vaccine.2019.07.074. Epub 2019 Aug 1.

DOI:10.1016/j.vaccine.2019.07.074
PMID:31378535
原文链接:https://pmc.ncbi.nlm.nih.gov/articles/PMC7182153/
Abstract

Vaccination offers the most cost-effective approach to limiting the adverse impact of infectious and neoplastic diseases that reduce the quality of life in sub-Saharan Africa (SSA). However, it is unclear what vaccine vectors would be most readily implementable in the setting and at what age they should be applied for maximal efficacy. Adenoviruses (Ad) and Ad-based vectors have been demonstrated to induce effective humoral and cellular immune responses in animal models and in humans. However, because immunity associated with Ad infection is lifelong, there exists a debate as to whether pre-existing immunity might decrease the efficacy of Ad vectored vaccines. In order to begin to rationally develop vaccination strategies for SSA, we have quantified neutralizing antibodies (nAb) against Ad4, Ad5, Ad7, Ad26, Ad28, Ad45 and Ad48 in 67 adult women and their infants. We are the first to define the decay kinetics of transferred maternal nAb in infants as well as the apparent initiation of de novo Ad responses. Our findings demonstrate that in Zambian adults, robust nAb responses exist against each of the Ads tested and are efficiently transferred to newborns. With few exceptions, neither the HIV-1 infection status of the mothers or the antiretroviral therapy (ART) treatment of HIV-1 disease had significant impact on maternal Ad nAb responses or their transfer to infants. However, maternal Ad nAb decays in infants to a nadir at 12 months of age such that any of the seven Ad types could function as vaccine vectors. The definition of this 'window of opportunity' provides important foundational data for rational design and implementation of Ad vectors in this setting.

摘要

接种疫苗是限制传染病和肿瘤疾病对撒哈拉以南非洲(SSA)地区生活质量负面影响的最具成本效益的方法。然而,尚不清楚在该地区最容易实施哪种疫苗载体,以及应该在什么年龄段应用才能达到最大效果。腺病毒(Ad)和基于 Ad 的载体已被证明可在动物模型和人类中诱导有效的体液和细胞免疫应答。然而,由于与 Ad 感染相关的免疫是终身的,因此存在一个争论,即预先存在的免疫是否会降低 Ad 载体疫苗的效果。为了开始为 SSA 合理制定疫苗接种策略,我们已经在 67 名成年女性及其婴儿中定量了针对 Ad4、Ad5、Ad7、Ad26、Ad28、Ad45 和 Ad48 的中和抗体(nAb)。我们首次定义了婴儿中转基因母体 nAb 的衰减动力学以及新出现的 Ad 反应的明显起始。我们的研究结果表明,在赞比亚成年人中,针对所测试的每种 Ad 都存在强大的 nAb 反应,并且可以有效地转移到新生儿。除了少数例外,母亲的 HIV-1 感染状况或 HIV-1 疾病的抗逆转录病毒治疗(ART)对母体 Ad nAb 反应或其向婴儿的转移均无明显影响。然而,婴儿中的母体 Ad nAb 会衰减至 12 个月时的最低点,以至于七种 Ad 类型中的任何一种都可以用作疫苗载体。该“窗口期”的定义为在该环境中合理设计和实施 Ad 载体提供了重要的基础数据。

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First-in-human randomized controlled trial of an oral, replicating adenovirus 26 vector vaccine for HIV-1.人类首次口服复制型 26 型腺病毒载体疫苗治疗 HIV-1 的随机对照临床试验
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Immunogenicity of adenovirus-vector vaccine targeting hepatitis B virus: non-clinical safety assessment in non-human primates.靶向乙型肝炎病毒的腺病毒载体疫苗的免疫原性:非人类灵长类动物的非临床安全性评估。
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