新型活流感疫苗M2SR可保护小鼠和雪貂免受高致病性禽流感的侵害。
M2SR, a novel live influenza vaccine, protects mice and ferrets against highly pathogenic avian influenza.
作者信息
Hatta Yasuko, Boltz David, Sarawar Sally, Kawaoka Yoshihiro, Neumann Gabriele, Bilsel Pamuk
机构信息
FluGen Inc., Madison, WI 53711, USA.
IIT Research Institute, Chicago, IL 60616, USA.
出版信息
Vaccine. 2017 Jul 24;35(33):4177-4183. doi: 10.1016/j.vaccine.2017.06.039. Epub 2017 Jun 28.
The emergence of highly pathogenic avian influenza H5N1 viruses has heightened global concern about the threat posed by pandemic influenza. To address the need for a highly effective universal influenza vaccine, we developed a novel M2-deficient single replication (M2SR) influenza vaccine virus and previously reported that it provided strong heterosubtypic protection against seasonal influenza viruses in mice. In the current study, we assessed M2SR induced protection against H5N1 influenza in mice and ferrets. Mice were intranasally inoculated with M2SR viruses containing the HA and NA from A/Vietnam/1203/2004 (M2SR H5N1) or A/California/07/2009 (M2SR H1N1). All M2SR vaccinated mice survived lethal challenge with influenza A/Vietnam/1203/2004 (H5N1), whereas 40% of mice vaccinated with recombinant H5 HA and none of the naïve controls survived. M2SR H5N1 provided sterile immunity, whereas low levels of virus were detected in the lungs of some M2SR H1N1 vaccinated mice. In contrast, recombinant H5 HA vaccinated mice and naïve controls showed systemic infection. M2SR H5N1 induced strong serum and mucosal antibody responses (IgG and IgA classes) against H5 HA, with high hemagglutination inhibition (HAI) titers. In contrast, while M2SR H1N1 elicited cross-reactive antibodies recognizing the H5 HA2 stalk region or the neuraminidase, no HAI activity against H5N1 virus was detected after M2SR H1N1 immunization. Both M2SR H5N1 and H1N1 also protected ferrets against lethal challenge with A/Vietnam/1203/2004. A prime-boost regimen provided optimal protection with no virus detected in the respiratory tract or brain after challenge. As in the mouse model, only the M2SR H5N1 vaccine induced HAI antibodies against the challenge virus in ferrets, while the M2SR H1N1 was able to provide protection without the induction of HAI antibodies. In summary, effective protection against highly pathogenic H5N1 influenza virus was provided by both homologous H5N1 M2SR and heterologous H1N1 M2SR demonstrating the cross-protective attributes of the M2SR platform.
高致病性H5N1禽流感病毒的出现加剧了全球对大流行性流感威胁的担忧。为满足对高效通用流感疫苗的需求,我们研发了一种新型的缺乏M2蛋白的单复制(M2SR)流感疫苗病毒,并且此前报道它在小鼠中对季节性流感病毒提供了强大的异源亚型保护。在当前研究中,我们评估了M2SR在小鼠和雪貂中诱导的针对H5N1流感的保护作用。将含有来自A/越南/1203/2004(M2SR H5N1)或A/加利福尼亚/07/2009(M2SR H1N1)的血凝素(HA)和神经氨酸酶(NA)的M2SR病毒经鼻内接种小鼠。所有接种M2SR疫苗的小鼠在接受甲型流感病毒A/越南/1203/2004(H5N1)的致死性攻击后存活,而接种重组H5 HA的小鼠中有40%死亡,未接种的对照小鼠全部死亡。M2SR H5N1提供了无菌免疫,而在一些接种M2SR H1N1疫苗的小鼠肺中检测到低水平病毒。相比之下,接种重组H5 HA的小鼠和未接种的对照小鼠出现了全身感染。M2SR H5N1诱导了针对H5 HA的强烈血清和黏膜抗体反应(IgG和IgA类),血凝抑制(HAI)效价高。相比之下,虽然M2SR H1N1引发了识别H5 HA2茎区或神经氨酸酶的交叉反应性抗体,但在M2SR H1N1免疫后未检测到针对H5N1病毒的HAI活性。M2SR H5N1和H1N1也保护雪貂免受甲型流感病毒A/越南/1203/2004的致死性攻击。一种初免 - 加强免疫方案提供了最佳保护,攻击后在呼吸道或脑中未检测到病毒。与小鼠模型一样,只有M2SR H5N1疫苗在雪貂中诱导了针对攻击病毒的HAI抗体,而M2SR H1N1能够在不诱导HAI抗体的情况下提供保护。总之,同源的H5N1 M2SR和异源的H1N1 M2SR都提供了针对高致病性H5N1流感病毒的有效保护,证明了M2SR平台的交叉保护特性。
Zotero 插件