Sequential immunization of macaques elicits heterologous neutralizing antibodies targeting the V3-glycan patch of HIV-1 Env

病毒学 异源的 抗体 免疫 中和抗体 聚糖 中和 人类免疫缺陷病毒(HIV) 艾滋病疫苗 免疫学 慢病毒 生物 医学 糖蛋白 疫苗试验 分子生物学 病毒性疾病 遗传学 基因
作者
Amelia Escolano,Harry B. Gristick,Rajeev Gautam,Andrew T. DeLaitsch,Morgan E. Abernathy,Zhi Yong Yang,Haoqing Wang,Magnus A.G. Hoffmann,Yoshiaki Nishimura,Zijun Wang,Nicholas Koranda,Leesa M. Kakutani,Han Gao,Priyanthi N. P. Gnanapragasam,Henna Raina,Ana Gazumyan,Melissa Cipolla,Thiago Y. Oliveira,Victor Ramos,Darrell J. Irvine,Murillo Silva,Anthony P. West,Jennifer R. Keeffe,Christopher O. Barnes,Michael S. Seaman,Michel C. Nussenzweig,Malcolm A. Martin,Pamela J. Bjorkman
出处
期刊:Science Translational Medicine [American Association for the Advancement of Science (AAAS)]
卷期号:13 (621) 被引量:22
标识
DOI:10.1126/scitranslmed.abk1533
摘要

Broadly neutralizing antibodies (bNAbs) against HIV-1 develop after prolonged virus and antibody coevolution. Previous studies showed that sequential immunization with a V3-glycan patch germline-targeting HIV-1 envelope trimer (Env) followed by variant Envs can reproduce this process in mice carrying V3-glycan bNAb precursor B cells. However, eliciting bNAbs in animals with polyclonal antibody repertoires is more difficult. We used a V3-glycan immunogen multimerized on virus-like particles (VLPs), followed by boosting with increasingly native-like Env-VLPs, to elicit heterologous neutralizing antibodies in nonhuman primates (NHPs). Structures of antibody/Env complexes after prime and boost vaccinations demonstrated target epitope recognition with apparent maturation to accommodate glycans. However, we also observed increasing off-target antibodies with boosting. Eight vaccinated NHPs were subsequently challenged with simian-human immunodeficiency virus (SHIV), and seven of eight animals became infected. The single NHP that remained uninfected after viral challenge exhibited one of the lowest neutralization titers against the challenge virus. These results demonstrate that more potent heterologous neutralization resulting from sequential immunization is necessary for protection in this animal model. Thus, improved prime-boost regimens to increase bNAb potency and stimulate other immune protection mechanisms are essential for developing anti–HIV-1 vaccines.
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