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接种疫苗可诱导新生恒河猴产生 HIV Env 特异性 IgG 抗体,并可在婴儿期通过晚期加强免疫来增强。

HIV Env-Specific IgG Antibodies Induced by Vaccination of Neonatal Rhesus Macaques Persist and Can Be Augmented by a Late Booster Immunization in Infancy.

机构信息

Department of Microbiology and Immunology, Center for AIDS Research, and Children's Research Institute, School of Medicine, University of North Carolina at Chapel Hill, Chapel Hill, North Carolina, USA.

Duke Human Vaccine Institute, Duke University Medical Center, Durham, North Carolina, USA.

出版信息

mSphere. 2020 Mar 25;5(2):e00162-20. doi: 10.1128/mSphere.00162-20.

Abstract

The HIV epidemics in infants and adolescent women are linked. Young women of childbearing age are at high risk for HIV infection and, due to poor HIV testing rates and low adherence to antiretroviral therapy, are at high risk for mother-to-infant transmission. We hypothesize that HIV vaccine regimens initiated in early life would provide the necessary time frame to induce mature and highly functional Env-specific antibody responses that could potentially also protect against HIV acquisition later in life. The present study was designed to test two vaccine regimens, a clade C HIV Env protein vaccine (Env only) alone or combined with a modified vaccinia Ankara (MVA) vector expressing HIV Env (MVA/Env) for the induction and persistence of Env-specific antibody responses in an infant nonhuman primate model. Vaccination was initiated within the first week of life, with booster immunizations at weeks 6, 12, and 32. We demonstrate that both vaccine strategies were able to elicit durable Env-specific antibody responses that were enhanced by a late boost in infancy. Furthermore, we confirmed earlier data that intramuscular administration of the Env protein with the Toll-like receptor 7/8 (TLR7/8)-based adjuvant 3M-052 in stable emulsion (3M-052-SE) induced higher Env-specific antibody responses than vaccination with Env adjuvanted in Span85-Tween 80-squalene (STS) tested in a previous study. These results support the concept of early vaccination as a means to induce durable immune responses that may prevent HIV infection in adolescence at the onset of sexual debut. The majority of new HIV-1 infections occur in young adults, with adolescent women being 3 times more likely to acquire HIV than young men. Implementation of HIV prevention strategies has been less successful in this age group; thus, a vaccine given prior to adolescence remains a high priority. We propose that instead of starting HIV vaccination during adolescence, an HIV vaccine regimen initiated in early infancy, aligned with the well-accepted pediatric vaccine schedule and followed with booster immunizations, will provide an alternative means to reduce HIV acquisition in adolescence. Importantly, the long window of time between the first infant vaccine dose and the adolescence vaccine dose will allow for the maturation of highly functional HIV Env-specific antibody responses. Our study provides evidence that early life vaccination induces durable Env-specific plasma IgG responses that can be boosted to further improve the quality of the antibody response.

摘要

婴儿和青春期女性中的 HIV 流行是相关的。生育年龄的年轻女性感染 HIV 的风险很高,由于 HIV 检测率低和抗逆转录病毒治疗依从性低,她们处于母婴传播的高风险中。我们假设,在生命早期启动的 HIV 疫苗方案将提供必要的时间框架,以诱导成熟且高度功能性的 Env 特异性抗体反应,这些反应也有可能预防以后生活中感染 HIV。本研究旨在测试两种疫苗方案,即单独的 clade C HIV Env 蛋白疫苗(仅 Env)或与表达 HIV Env 的改良痘苗安卡拉(MVA)载体(MVA/Env)联合使用,以在婴儿非人灵长类动物模型中诱导和维持 Env 特异性抗体反应。疫苗接种在生命的第一周内开始,在第 6、12 和 32 周进行加强免疫。我们证明,这两种疫苗策略都能够引起持久的 Env 特异性抗体反应,并且在婴儿期后期加强免疫可以增强这种反应。此外,我们证实了早期数据,即在稳定乳液中使用 TLR7/8 (TLR7/8)为基础的佐剂 3M-052 (3M-052-SE)肌肉内给药的 Env 蛋白比在以前的研究中用 Span85-Tween 80-角鲨烯(STS)佐剂的 Env 疫苗接种诱导更高的 Env 特异性抗体反应。这些结果支持早期接种疫苗以诱导持久免疫反应的概念,这种反应可能会预防青春期性初潮时感染 HIV。大多数新的 HIV-1 感染发生在年轻人中,青春期女性感染 HIV 的可能性比年轻男性高 3 倍。在这个年龄组中,HIV 预防策略的实施效果较差;因此,在青春期前接种疫苗仍然是当务之急。我们建议,而不是在青春期开始 HIV 疫苗接种,在婴儿早期开始的 HIV 疫苗方案,与公认的儿科疫苗接种计划一致,并进行加强免疫,将提供一种替代方法来减少青春期的 HIV 感染。重要的是,从婴儿第一剂疫苗到青春期疫苗之间的长窗口期将允许高度功能性的 HIV Env 特异性抗体反应成熟。我们的研究提供了证据,表明早期生活疫苗接种会引起持久的 Env 特异性血浆 IgG 反应,可以加强这些反应,进一步提高抗体反应的质量。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/3264/7096624/2f5d3907b7b6/mSphere.00162-20-f0001.jpg

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