SARS-CoV-2 穗状病毒样颗粒含有流感 H1/N1 抗原,可诱导小鼠产生双重免疫力。

Vaccine Pub Date : 2024-12-02 Epub Date: 2024-10-30 DOI:10.1016/j.vaccine.2024.126463
Zalma V Sanchez-Martinez, Sergio P Alpuche-Lazcano, Matthew Stuible, Bassel Akache, Tyler M Renner, Lise Deschatelets, Renu Dudani, Blair A Harrison, Michael J McCluskie, Sabahudin Hrapovic, Julie Blouin, Xinyu Wang, Matthew Schuller, Kai Cui, Jae-Young Cho, Yves Durocher
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摘要

一种同时对 SARS-CoV-2 和甲型流感 (IAV) 病毒有效的疫苗可能是一种具有成本效益的策略,可减轻这两种病毒对公众健康造成的综合负担,并减少同时感染可能引起的并发症。基于之前发现的全长 SARS-CoV-2 棘突(S)表达能诱导 CHO 细胞产生高水平的包膜 VLP(eVLP),我们测试了 IAV H1N1 血凝素(H1)和神经氨酸酶(N1)是否也能在这些颗粒上显示。我们发现,IAV 表面抗原在尖峰 VLPs(S-VLPs)中的共结合是非常有效的:在 CHO 细胞中瞬时共表达 S + H1 或 S + H1 + N1 后,产生的 VLPs 含有相似数量的 SARS-CoV-2 S 抗原和 IAV 抗原。释放到培养基中的自组装二价(S/H1)和三价(S/H1/N1)VLPs通过使用S-VLP亲和树脂进行单步层析纯化。对纯化的VLPs进行的Western印迹分析和免疫金标记透射电子显微镜(TEM)证实,S、H1和N1抗原共存于同一颗粒中。最后,我们证明了在小鼠模型中,两种剂量的二价和三价 VLPs 佐剂能诱导特异性功能抗体和细胞免疫,这表明了 SARS-CoV-2/IAV 联合疫苗开发的潜力。
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SARS-CoV-2 spike-based virus-like particles incorporate influenza H1/N1 antigens and induce dual immunity in mice.

A vaccine effective against both SARS-CoV-2 and influenza A (IAV) viruses could represent a cost-effective strategy to reduce their combined public health burden as well as potential complications arising from co-infection. Based on previous findings that full-length SARS-CoV-2 spike (S) expression can induce high-level, enveloped VLP (eVLP) production in CHO cells, we tested whether IAV H1N1 hemagglutinin (H1) and neuraminidase (N1) could also be displayed on these particles. We found that co-incorporation of the IAV surface antigens in spike VLPs (S-VLPs) was highly efficient: upon transient co-expression of S + H1 or S + H1 + N1 in CHO cells, the resulting VLPs contained similar amounts of the SARS-CoV-2 S and IAV antigens. The self-assembled bivalent (S/H1) and trivalent (S/H1/N1) VLPs released into the culture media were purified by single-step chromatography using a S-VLP affinity resin. Western blot analysis and immuno‑gold labeling transmission electron microscopy (TEM) of purified VLPs confirmed the coexistence of S, H1 and N1 antigens in the same particles. Finally, we demonstrated that two doses of adjuvanted bivalent and trivalent VLPs elicit specific functional antibodies and cellular immunity in a mouse model, suggesting potential for combined SARS-CoV-2/IAV vaccine development.

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