University of Michigan, Michigan Nanotechnology Institute for Medicine and Biological Sciences (M-NIMBs), Ann Arbor, MI, United States.
BlueWillow Biologic, Ann Arbor, MI, United States.
Vaccine. 2019 Mar 14;37(12):1591-1600. doi: 10.1016/j.vaccine.2019.02.002. Epub 2019 Feb 19.
Highly pathogenic H5N1 influenza viruses remain a pandemic risk to the world population. Although vaccines are the best solution to prevent this threat, a more effective vaccine for H5 strains of influenza has yet to be developed. All existing vaccines target only serum antibody against influenza as the primary outcome, while mucosal immunity has not been addressed. To address these shortcomings we have used an effective mucosal adjuvant system to produce a prototype vaccine that provides antibody, cellular and mucosal immunity to multiple serotypes of H5.
Plant-derived recombinant H5 (rH5) antigen was mixed with a novel nanoemulsion NE01 adjuvant. The rH5-NE01 vaccine was administered intranasally to CD-1 mice and ferrets. Immunogenicity of this immunization was evaluated through rH5-specific antibody and cellular immune responses. Hemagglutination inhibition (HI) and virus neutralization (VN) assays were performed. Protection against H5N1 virus challenge was evaluated in ferrets.
Intranasal immunization with rH5-NE01vaccine induced high titers (>10) of rH5-specific IgG in mice. In mice and ferrets this vaccine also achieved titers of ≥40 for both HI and VN. Additionally, the levels of rH5-specific IgA were significantly increased in bronchial secretions in these animals. The rH5-NE01 vaccine enhanced rH5-specific cellular immune responses including IFN-γ and IL-17. Ten-day survival post challenge was 100% in ferrets that received rH5-NE01compared to 12.5% in the PBS group. Furthermore, this vaccine prevented weight loss and increases in body temperature after H5N1 challenge as compared to the controls. Moreover, H5N1 virus in nasal wash of rH5-NE01-vaccinated ferrets was significantly decreased compared to controls.
Intranasal immunization with rH5 antigen formulated with NE01 adjuvant elicited strong, broad and balanced immune responses that effectively protect against H5N1 influenza virus infection in the ferret model. The ease of formulation of rH5-NE01 makes this novel combination a promising mucosal vaccine candidate for pandemic influenza.
高致病性 H5N1 流感病毒仍然对世界人口构成大流行风险。虽然疫苗是预防这一威胁的最佳解决方案,但尚未开发出针对 H5 流感株更有效的疫苗。所有现有的疫苗都仅以血清抗体作为流感的主要治疗效果指标,而忽视了黏膜免疫。为了解决这些缺点,我们使用了一种有效的黏膜佐剂系统来生产一种原型疫苗,该疫苗可针对多种 H5 血清型提供抗体、细胞和黏膜免疫。
植物源性重组 H5(rH5)抗原与新型纳米乳 NE01 佐剂混合。rH5-NE01 疫苗经鼻腔内给药给 CD-1 小鼠和雪貂。通过 rH5 特异性抗体和细胞免疫反应评估这种免疫接种的免疫原性。进行血凝抑制(HI)和病毒中和(VN)测定。在雪貂中评估对 H5N1 病毒攻击的保护作用。
rH5-NE01 疫苗鼻腔内免疫可诱导小鼠体内 rH5 特异性 IgG 滴度(>10)升高。在小鼠和雪貂中,该疫苗还可实现 HI 和 VN 的滴度均≥40。此外,在这些动物的支气管分泌物中 rH5 特异性 IgA 水平显著增加。rH5-NE01 疫苗增强了 rH5 特异性细胞免疫反应,包括 IFN-γ和 IL-17。接受 rH5-NE01 疫苗的雪貂在 10 天攻毒后 100%存活,而 PBS 组为 12.5%。此外,与对照组相比,该疫苗可预防 H5N1 攻击后体重减轻和体温升高。此外,与对照组相比,rH5-NE01 疫苗接种的雪貂鼻洗液中的 H5N1 病毒显著减少。
rH5 抗原与 NE01 佐剂联合鼻腔内免疫可引起强烈、广泛和平衡的免疫反应,可有效保护雪貂免受 H5N1 流感病毒感染。rH5-NE01 的配方简单,使其成为一种有前途的大流行性流感黏膜候选疫苗。
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