基于镶嵌血凝素方法的通用乙型流感灭活疫苗的临床前评估。

IF 6.9 1区 医学 Q1 IMMUNOLOGY
Irene González-Domínguez, Eduard Puente-Massaguer, Adam Abdeljawad, Tsoi Ying Lai, Yonghong Liu, Madhumathi Loganathan, Benjamin Francis, Nicholas Lemus, Victoria Dolange, Marta Boza, Stefan Slamanig, Jose Luis Martínez-Guevara, Florian Krammer, Peter Palese, Weina Sun
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引用次数: 0

摘要

我们开发了一种新的通用乙型流感疫苗接种策略,该策略以显示马赛克血凝素(mHA)的灭活乙型流感病毒为基础。重组 mHA 病毒是用外来禽流感甲型流感病毒 HA 的四个主要抗原位点取代乙型流感病毒 HA 的四个主要抗原位点而构建的。与接种野生型病毒相比,用基于 mHA 的疫苗连续接种天真小鼠可对 HA 的免疫亚优势保守表位产生更高的免疫反应。在测试的不同制剂中,mHA 分体疫苗的免疫原性低于全灭活病毒疫苗。使用 Toll 样受体-9 激动剂(CpG 1018)佐剂的 mHA 分裂疫苗增强了 Th1 免疫和体内交叉保护,而使用 MF59 样水包油纳米乳剂(AddaVax)佐剂则增强并扩大了体液免疫反应和抗体介导的交叉保护。随后,我们在先前免疫过的小鼠身上评估了含佐剂或不含佐剂的 mHA 疫苗,以近似模拟人类对乙型流感病毒的原有免疫力,并在此模型中评估了先天免疫和细胞免疫的贡献。我们相信,这些采用 mHA 策略的临床前研究是朝着在临床试验中评估通用乙型流感病毒疫苗迈出的重要一步。
本文章由计算机程序翻译,如有差异,请以英文原文为准。
Preclinical evaluation of a universal inactivated influenza B vaccine based on the mosaic hemagglutinin-approach.

We have developed a new universal influenza B vaccination strategy based on inactivated influenza B viruses displaying mosaic hemagglutinins (mHAs). Recombinant mHA viruses were constructed by replacing the four major antigenic sites of influenza B virus HAs, with those from exotic avian influenza A virus HAs. Sequential vaccination of naïve mice with mHA-based vaccines elicited higher immune responses towards the immuno-subdominant conserved epitopes of the HA than vaccination with wildtype viruses. Among the different preparations tested, mHA split vaccines were less immunogenic than their whole inactivated virus counterparts. This lower immunogenicity was overcome by the combination with adjuvants. mHA split vaccines adjuvanted with a Toll-like receptor-9 agonist (CpG 1018) increased Th1 immunity and in vivo cross-protection, whereas adjuvanting with an MF59-like oil-in-water nano-emulsion (AddaVax) enhanced and broadened humoral immune responses and antibody-mediated cross-protection. The mHA vaccines with or without adjuvant were subsequently evaluated in mice that were previously immunized to closely mimic human pre-existing immunity to influenza B viruses and the contribution of innate and cellular immunity was evaluated in this model. We believe these preclinical studies using the mHA strategy represent a major step toward the evaluation of a universal influenza B virus vaccine in clinical trials.

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来源期刊
NPJ Vaccines
NPJ Vaccines Immunology and Microbiology-Immunology
CiteScore
11.90
自引率
4.30%
发文量
146
审稿时长
11 weeks
期刊介绍: Online-only and open access, npj Vaccines is dedicated to highlighting the most important scientific advances in vaccine research and development.
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