IFITM3-deficient mice as a model for testing influenza virus vaccines via the intramuscular route

IF 4.5 3区医学 Q2 IMMUNOLOGY

Vaccine Pub Date : 2025-07-08 DOI:10.1016/j.vaccine.2025.127458

Adrian C. Eddy , Samuel Speaks , Megan Roth, Jack E. Roettger, Brendan M. Reznik, Shreenath Mohan, Ben D. Liu, Emily A. Hemann, Jacob S. Yount

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Abstract

Influenza virus infections remain a significant global health concern. Development of a universal influenza vaccine has been met with challenges, in part due to difficulties with preclinical vaccine testing in mice, which are widely available but are often poorly infected with human and avian influenza viruses. Here, we investigate whether mice lacking interferon-induced transmembrane protein 3 (IFITM3), an antiviral restriction factor, provide a suitable preclinical model for vaccine testing since we observe enhanced replication of multiple influenza virus strains in these mice. We find that IFITM3 KO mice produce a blunted antibody response to intramuscular vaccination that is increased by a booster dose. Nonetheless, their adaptive immune responses to previous infections and vaccinations were found to be functional in limiting weight loss, survival, and viral replication in challenge studies. Overall, our findings identify IFITM3 KO mice as an accessible, functionally immunocompetent preclinical model for assessment of influenza vaccines.

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ifitm3缺陷小鼠作为流感病毒疫苗通过肌肉注射途径测试的模型

流感病毒感染仍然是一个重大的全球卫生问题。研制一种通用流感疫苗遇到了挑战，部分原因是在小鼠身上进行临床前疫苗试验存在困难，这些小鼠广泛存在，但往往很少感染人流感病毒和禽流感病毒。在这里，我们研究缺乏干扰素诱导的跨膜蛋白3 （IFITM3）的小鼠是否为疫苗试验提供了合适的临床前模型，因为我们观察到这些小鼠中多种流感病毒株的复制增强。IFITM3是一种抗病毒限制因子。我们发现IFITM3 KO小鼠对肌肉注射疫苗产生钝化的抗体反应，这种反应通过加强剂量增加。尽管如此，在挑战研究中，他们对先前感染和疫苗接种的适应性免疫反应被发现在限制体重减轻、生存和病毒复制方面起作用。总的来说，我们的研究结果确定IFITM3 KO小鼠是一种可获得的、功能免疫能力强的流感疫苗评估临床前模型。

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

Vaccine 医学-免疫学

CiteScore

8.70

自引率

5.50%

发文量

992

审稿时长

131 days

期刊介绍： Vaccine is unique in publishing the highest quality science across all disciplines relevant to the field of vaccinology - all original article submissions across basic and clinical research, vaccine manufacturing, history, public policy, behavioral science and ethics, social sciences, safety, and many other related areas are welcomed. The submission categories as given in the Guide for Authors indicate where we receive the most papers. Papers outside these major areas are also welcome and authors are encouraged to contact us with specific questions.