Immunofocusing on the conserved fusion peptide of HIV envelope glycoprotein in rhesus macaques.

以恒河猴 HIV 包膜糖蛋白的保守融合肽为研究对象进行免疫聚焦

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作者:Pratap Payal P, Cottrell Christopher A, Quinn James, Carnathan Diane G, Bader Daniel L V, Tran Andy S, Enemuo Chiamaka A, Ngo Julia T, Richey Sara T, Gao Hongmei, Shen Xiaoying, Greene Kelli M, Hurtado Jonathan, Michaels Katarzyna Kaczmarek, Ben-Akiva Elana, Lemnios Ashley, Melo Mariane B, Allen Joel D, Ozorowski Gabriel, Crispin Max, Briney Bryan, Montefiori David, Silvestri Guido, Irvine Darrell J, Crotty Shane, Ward Andrew B
During infection, the fusion peptide (FP) of HIV envelope glycoprotein (Env) serves a central role in viral fusion with the host cell. As such, the FP is highly conserved and therefore an attractive epitope for vaccine design. Here, we describe a vaccination study in non-human primates (NHPs) where glycan deletions were made on soluble HIV Env to increase FP epitope exposure. When delivered via implantable osmotic pumps, this immunogen primed immune responses against the FP, which were then boosted with heterologous trimers resulting in a focused immune response targeting the conserved FP epitope. Although autologous immunizations did not elicit high affinity FP-targeting antibodies, the conserved FP epitope on a heterologous trimer further matured the lower affinity, FP-targeting B cells. This study suggests using epitope conservation strategies on distinct Env trimer immunogens can focus humoral responses on desired neutralizing epitopes and suppress immune-distracting antibody responses against non-neutralizing epitopes.

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