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基于猪 H1N1 流感血凝素序列的计算优化广谱反应性疫苗可预防猪源性和人源性分离病毒。

Computationally optimized broadly reactive vaccine based upon swine H1N1 influenza hemagglutinin sequences protects against both swine and human isolated viruses.

机构信息

Center for Vaccines and Immunology, University of Georgia , Athens , GA , USA.

Vaccine and Gene Therapy Institute of Florida , Port St. Lucie , FL , USA.

出版信息

Hum Vaccin Immunother. 2019;15(9):2013-2029. doi: 10.1080/21645515.2019.1653743.

Abstract

Swine H1 influenza viruses were stable within pigs for nearly 70 years until in 1998 when a classical swine virus reassorted with avian and human influenza viruses to generate the novel triple reassortant H1N1 strain that eventually led to the 2009 influenza pandemic. Previously, our group demonstrated broad protection against a panel of human H1N1 viruses using HA antigens derived by the COBRA methodology. In this report, the effectiveness of COBRA HA antigens (SW1, SW2, SW3 and SW4), which were designed using only HA sequences from swine H1N1 and H1N2 isolates, were tested in BALB/c mice. The effectiveness of these vaccines were compared to HA sequences designed using both human and swine H1 HA sequences or human only sequences. SW2 and SW4 elicited antibodies that detected the pandemic-like virus, A/California/07/2009 (CA/09), had antibodies with HAI activity against almost all the classical swine influenza viruses isolated from 1973-2015 and all of the Eurasian viruses in our panel. However, sera collected from mice vaccinated with SW2 or SW4 had HAI activity against ~25% of the human seasonal-like influenza viruses isolated from 2009-2015. In contrast, the P1 COBRA HA vaccine (derived from both swine and human HA sequences) elicited antibodies that had HAI activity against both swine and human H1 viruses and protected against CA/09 challenge, but not a human seasonal-like swine H1N2 virus challenge. However, the SW1 vaccine protected against this challenge as well as the homologous vaccine. These results support the idea that a pan-swine-human H1 influenza virus vaccine is possible.

摘要

猪源 H1 流感病毒在猪体内稳定存在了近 70 年,直到 1998 年,一种经典的猪流感病毒与禽源和人流感病毒重配,产生了新型的三重重配 H1N1 毒株,最终导致了 2009 年的流感大流行。在此之前,我们的研究小组使用 COBRA 方法学衍生的 HA 抗原,对一组人源 H1N1 病毒进行了广泛的保护研究。在本报告中,我们测试了仅使用猪源 H1N1 和 H1N2 分离株的 HA 序列设计的 COBRA HA 抗原(SW1、SW2、SW3 和 SW4)在 BALB/c 小鼠中的有效性。这些疫苗的有效性与使用人源和猪源 HA 序列或仅人源序列设计的 HA 序列进行了比较。SW2 和 SW4 诱导的抗体可检测到类似大流行的病毒 A/California/07/2009(CA/09),对 1973-2015 年分离的几乎所有经典猪流感病毒以及我们组中所有欧亚病毒具有血凝抑制(HAI)活性。然而,用 SW2 或 SW4 免疫的小鼠血清对 2009-2015 年分离的约 25%的人季节性流感病毒具有 HAI 活性。相比之下,P1 COBRA HA 疫苗(源自猪源和人源 HA 序列)诱导的抗体对猪源和人源 H1 病毒均具有 HAI 活性,并能抵抗 CA/09 的攻击,但不能抵抗人源季节性猪源 H1N2 病毒的攻击。然而,SW1 疫苗不仅能抵抗这种挑战,还能抵抗同源疫苗。这些结果支持了一种泛猪源-人源 H1 流感病毒疫苗是可能的想法。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/ea03/6773400/e83d72dfa530/khvi-15-09-1653743-g001.jpg

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