首页> 外文期刊>Cellular Physiology and Biochemistry >The Protective Effects of the A/ZJU01/ PR8/2013 Split H7N9 Avian Influenza Vaccine Against Highly Pathogenic H7N9 in BALB/c Mice
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The Protective Effects of the A/ZJU01/ PR8/2013 Split H7N9 Avian Influenza Vaccine Against Highly Pathogenic H7N9 in BALB/c Mice

机译:A / ZJU01 / PR8 / 2013分离的H7N9禽流感疫苗对BALB / c小鼠中高致病性H7N9的保护作用

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Background/Aims Since the first case of novel H7N9 infection was reported, China has experienced five epidemics of H7N9. During the fifth wave, a highly pathogenic H7N9 strain emerged. In order to assess whether the H7N9 vaccine based on A/Zhejiang/DTID-ZJU01/2013(H7N9) was effective in protecting against highly pathogenic H7N9, we conducted this study. Methods Groups of mice were immunized twice by intraperitoneal injection with 500 µl of either split vaccine alone or MF59-adjuvanted vaccine. Serum was collected 2 weeks after the second vaccine booster. The hemagglutinin inhibition test was conducted on vaccine seed and highly pathogenic H7N9 to evaluate the neutralization of highly pathogenic H7N9. We also immunized mice and challenged them with highly pathogenic H7N9. Mice were observed for illness, weight loss, and death at 1 week and 2 weeks post-infection. Then, the mice were sacrificed and lungs were removed. Antibody responses were assessed and pathological changes in the lung tissue were evaluated. Results The ability of serum to neutralize highly pathogenic H7N9 was reduced. In mice, highly pathogenic H7N9 was more virulent than A/Zhejiang/DTID-ZJU01/2013(H7N9). After challenge with highly pathogenic H7N9, all mice died while mice challenged with A/Zhejiang/DTID-ZJU01/2013(H7N9) all recovered. The A/ZJU01/PR8/2013 split H7N9 avian influenza vaccine was able to protect against infection with highly pathogenic H7N9 in mice, with or without MF59. Moreover, H7N9 vaccine adjuvanted with MF59 produced high antibody levels, which lead to better protection. Conclusions The A/ZJU01/PR8/2013 split H7N9 avian influenza vaccine based on A/Zhejiang/DTID-ZJU01/2013(H7N9) is effective in protecting against highly pathogenic H7N9. H7N9 vaccine adjuvanted with MF59 offers better protection against infection with highly pathogenic H7N9. In order to make the H7N9 vaccine applicable to humans, further clinical trials are required to evaluate MF59 adjuvanted vaccine. Meanwhile, the vaccine strain should be updated based on the highly pathogenic H7N9 gene sequence.
机译:背景/目的自从报道第一例新型H7N9感染以来,中国经历了5次H7N9流行病。在第五波期间,出现了高致病性的H7N9菌株。为了评估基于A / Zhejiang / DTID-ZJU01 / 2013(H7N9)的H7N9疫苗在预防高致病性H7N9方面是否有效,我们进行了这项研究。方法通过腹膜内注射500μl单独的分裂疫苗或MF59辅助疫苗对小鼠组进行两次免疫。在第二次疫苗加强免疫后2周收集血清。对疫苗种子和高致病性H7N9进行血凝素抑制试验,以评估高致病性H7N9的中和作用。我们还免疫了小鼠,并用高致病性H7N9攻击了它们。在感染后1周和2周观察小鼠的疾病,体重减轻和死亡。然后,处死小鼠并去除肺。评估抗体反应并评估肺组织的病理变化。结果降低了血清中和高致病性H7N9的能力。在小鼠中,高致病性H7N9比A / Zhejiang / DTID-ZJU01 / 2013(H7N9)更具毒性。在用高致病性H7N9攻击后,所有小鼠死亡,而用A / Zhejiang / DTID-ZJU01 / 2013(H7N9)攻击的小鼠全部恢复。 A / ZJU01 / PR8 / 2013分离的H7N9禽流感疫苗能够保护具有或不含MF59的小鼠感染高致病性H7N9。此外,佐以MF59的H7N9疫苗可产生高抗体水平,从而提供更好的保护。结论基于A / Zhejiang / DTID-ZJU01 / 2013(H7N9)的A / ZJU01 / PR8 / 2013分离的H7N9禽流感疫苗可有效预防高致病性H7N9。佐以MF59的H7N9疫苗可为高致病性H7N9感染提供更好的保护。为了使H7N9疫苗适用于人类,需要进一步的临床试验来评估MF59佐剂疫苗。同时,应根据高致病性H7N9基因序列更新疫苗株。

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