Disulfide-stabilized trimeric hemagglutinin ectodomains provide enhanced heterologous influenza protection.

IF 8.4 2区 医学 Q1 IMMUNOLOGY
Emerging Microbes & Infections Pub Date : 2024-12-01 Epub Date: 2024-08-18 DOI:10.1080/22221751.2024.2389095
De-Jian Liu, Xiu-Qin Zhong, Yan-Xia Ru, Shi-Long Zhao, Cui-Cui Liu, Yi-Bo Tang, Xuan Wu, Yi-Shuai Zhang, Hui-Hui Zhang, Jia-Yue She, Mu-Yang Wan, Yao-Wang Li, He-Ping Zheng, Lei Deng
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Abstract

Influenza virus infection poses a continual menace to public health. Here, we developed soluble trimeric HA ectodomain vaccines by establishing interprotomer disulfide bonds in the stem region, which effectively preserve the native antigenicity of stem epitopes. The stable trimeric H1 ectodomain proteins exhibited higher thermal stabilities in comparison with unmodified HAs and showed strong binding activities towards a panel of anti-stem cross-reactive antibodies that recognize either interprotomer or intraprotomer epitopes. Negative stain transmission electron microscopy (TEM) analysis revealed the stable trimer architecture of the interprotomer disulfide-stapled WA11#5, NC99#2, and FLD#1 proteins as well as the irregular aggregation of unmodified HA molecules. Immunizations of mice with those trimeric HA ectodomain vaccines formulated with incomplete Freund's adjuvant elicited significantly more potent cross-neutralizing antibody responses and offered broader immuno-protection against lethal infections with heterologous influenza strains compared to unmodified HA proteins. Additionally, the findings of our study indicate that elevated levels of HA stem-specific antibody responses correlate with strengthened cross-protections. Our design strategy has proven effective in trimerizing HA ectodomains derived from both influenza A and B viruses, thereby providing a valuable reference for designing future influenza HA immunogens.

二硫化物稳定的三聚体血凝素外结构域可提供更强的异源流感保护。
流感病毒感染对公众健康构成持续威胁。在此,我们通过在茎区建立原体间二硫键,开发了可溶性三聚体 HA 外结构域疫苗,从而有效地保留了茎表位的原生抗原性。与未修饰的HA相比,稳定的三聚体H1外结构域蛋白具有更高的热稳定性,并对识别茎间或茎内表位的抗茎交叉反应抗体具有很强的结合活性。负染色透射电子显微镜(TEM)分析显示,原体间二硫键结合的 WA11#5、NC99#2 和 FLD#1 蛋白具有稳定的三聚体结构,而未修饰的 HA 分子则呈不规则聚集。与未修饰的HA蛋白相比,用不完全弗罗因德佐剂配制的这些三聚体HA外结构域疫苗免疫小鼠可引起更强的交叉中和抗体反应,并在异源流感毒株的致命感染中提供更广泛的免疫保护。此外,我们的研究结果表明,HA 干特异性抗体反应水平的升高与交叉保护作用的加强相关。事实证明,我们的设计策略能有效地将来自甲型和乙型流感病毒的 HA 外结构域三聚化,从而为设计未来的流感 HA 免疫原提供有价值的参考。
本文章由计算机程序翻译,如有差异,请以英文原文为准。
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来源期刊
Emerging Microbes & Infections
Emerging Microbes & Infections IMMUNOLOGY-MICROBIOLOGY
CiteScore
26.20
自引率
2.30%
发文量
276
审稿时长
20 weeks
期刊介绍: Emerging Microbes & Infections is a peer-reviewed, open-access journal dedicated to publishing research at the intersection of emerging immunology and microbiology viruses. The journal's mission is to share information on microbes and infections, particularly those gaining significance in both biological and clinical realms due to increased pathogenic frequency. Emerging Microbes & Infections is committed to bridging the scientific gap between developed and developing countries. This journal addresses topics of critical biological and clinical importance, including but not limited to: - Epidemic surveillance - Clinical manifestations - Diagnosis and management - Cellular and molecular pathogenesis - Innate and acquired immune responses between emerging microbes and their hosts - Drug discovery - Vaccine development research Emerging Microbes & Infections invites submissions of original research articles, review articles, letters, and commentaries, fostering a platform for the dissemination of impactful research in the field.
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