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使用糖基工程化甲病毒样颗粒的新型HIV-1融合肽免疫原。

Novel HIV-1 fusion peptide immunogens using glycan-engineered alphavirus-like particles.

作者信息

Oh Seo-Ho, Gudipati Dedeepya R, Shi Wei, Zhao Peng, Wu Winston, Boyington Jeffrey C, Nariya Hardik K, McGhee Emily G, Azzam Tala, Raghunathan Vedhika, Yang Chumeng, Yang Catherine, Lee Christian, Kim Jane D, Zhou Tongqing, Mascola John R, Wells Lance, Kong Rui

出版信息

bioRxiv. 2025 May 5:2025.05.02.651772. doi: 10.1101/2025.05.02.651772.

DOI:10.1101/2025.05.02.651772
PMID:40568149
原文链接:https://pmc.ncbi.nlm.nih.gov/articles/PMC12190913/
Abstract

UNLABELLED

Immunofocusing on conserved, subdominant epitopes is critical for vaccines against highly diverse viruses such as HIV-1, influenza, and SARS-CoV-2. The eight-residue N-terminus of the HIV-1 fusion peptide (FP) is one such example of a promising yet small target. We developed new FP immunogens using three alphavirus-like particles (VLPs) and introduced additional glycans to mask shared carrier-specific epitopes. In two independent guinea pig studies, sequential immunization with heterologous carriers enhanced FP-directed antibody titers, which were further improved with glycan engineering. Separately, using diverse FP variants sharing the same N-terminal six amino acids increased neutralizing antibody titers. When combined, these two strategies led to higher FP-directed titers and, after Env trimer boosting, induced FP-directed neutralizing antibodies against multi-clade wild-type HIV-1 in nearly all animals. These findings established the importance of minimizing recurrent off-target epitopes across immunizations and support the engineered VLPs as a promising platform for peptide immunization.

HIGHLIGHTS

Novel HIV-1 fusion peptide immunogens using glycan-engineered alphavirus-like particlesImproved FP-directed response by minimizing recurrent carrier-specific epitopes across immunizationsImproved neutralizing response by sequential immunization with diverse FP variantsFP-directed antibodies neutralizing multi-clade wildtype viruses in nearly all animals.

摘要

未标记

针对保守的、亚显性表位进行免疫聚焦对于针对高度多样化病毒(如HIV-1、流感病毒和SARS-CoV-2)的疫苗至关重要。HIV-1融合肽(FP)的八残基N端就是这样一个有前景但较小的靶点的例子。我们使用三种类甲病毒颗粒(VLP)开发了新的FP免疫原,并引入额外的聚糖以掩盖共同的载体特异性表位。在两项独立的豚鼠研究中,用异源载体进行序贯免疫提高了针对FP的抗体滴度,通过聚糖工程进一步提高了抗体滴度。另外,使用共享相同N端六个氨基酸的不同FP变体提高了中和抗体滴度。当这两种策略结合使用时,导致更高的针对FP的滴度,并且在Env三聚体加强免疫后,几乎在所有动物中诱导出针对多亚型野生型HIV-1的针对FP的中和抗体。这些发现确立了在免疫过程中尽量减少反复出现的脱靶表位的重要性,并支持工程化VLP作为肽免疫的一个有前景的平台。

亮点

使用聚糖工程化类甲病毒颗粒的新型HIV-1融合肽免疫原通过在免疫过程中尽量减少反复出现的载体特异性表位来改善针对FP的反应通过用不同的FP变体进行序贯免疫来改善中和反应针对FP的抗体在几乎所有动物中中和多亚型野生型病毒。