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疫苗中的疫苗:4型和7型腺病毒作为流感疫苗载体的应用

Vaccines within vaccines: the use of adenovirus types 4 and 7 as influenza vaccine vectors.

作者信息

Weaver Eric A

机构信息

Division of Infectious Diseases; Mayo Clinic; Rochester, MN USA.

出版信息

Hum Vaccin Immunother. 2014;10(3):544-56. doi: 10.4161/hv.27238. Epub 2013 Nov 26.

Abstract

Adenovirus Types 4 and 7 (Ad4 and Ad7) are associated with acute respiratory distress (ARD). In order to prevent widespread Ad-associated ARD (Ad-ARD) the United States military immunizes new recruits using a safe and effective lyophilized wildtype Ad4 and Ad7 delivered orally in an enteric-coated capsule. We cloned Ad4 and Ad7 and modified them to express either a GFP-Luciferase (GFPLuc) fusion gene or a centralized influenza H1 hemagglutinin (HA1-con). BALB/c mice were injected with GFPLuc expressing viruses intramuscularly (i.m.) and intranasally (i.n.). Ad4 induced significantly higher luciferase expression levels as compared with Ad7 by both routes. Ad7 transduction was restored using a human CD46+ transgenic mouse model. Mice immunized with serial dilutions of viruses expressing the HA1-con influenza vaccine gene were challenged with 100 MLD 50 of influenza virus. Ad4 protected BALB/c mice at a lower dose by i.m. immunization as compared with Ad7. Unexpectedly, there was no difference in protection by i.n. immunization. Although Ad7 i.m. transduction was restored in CD46+ transgenic mice, protection against influenza challenge required even higher doses as compared with the BALB/c mice. However, Ad7 i.n. immunized CD46+ transgenic mice were better protected as compared with Ad4. Interestingly, the restoration of Ad7 transduction in CD46+ mice did not increase vaccine efficacy and indicates that Ad7 may transduce a different subset of cells through alternative receptors in the absence of CD46. These data indicate that both Ad4 and Ad7 can effectively induce anti-H1N1 immunity against a heterologous challenge using a centralized H1 gene. Future studies in non-human primates or human clinical trials will determine the overall effectiveness of Ad4 and Ad7 as vaccines for influenza.

摘要

4型和7型腺病毒(Ad4和Ad7)与急性呼吸窘迫(ARD)有关。为预防广泛的腺病毒相关急性呼吸窘迫(Ad-ARD),美国军方使用一种安全有效的冻干野生型Ad4和Ad7,通过肠溶胶囊口服免疫新兵。我们克隆了Ad4和Ad7,并对它们进行改造以表达绿色荧光蛋白-荧光素酶(GFP-Luc)融合基因或集中化的甲型流感病毒H1血凝素(HA1-con)。将表达GFP-Luc的病毒通过肌肉注射(i.m.)和鼻内注射(i.n.)接种到BALB/c小鼠体内。两种接种途径下,Ad4诱导的荧光素酶表达水平均显著高于Ad7。使用人CD46+转基因小鼠模型恢复了Ad7的转导。用表达HA1-con流感疫苗基因的病毒系列稀释液免疫的小鼠,用100 MLD 50的流感病毒进行攻击。与Ad7相比,Ad4通过肌肉注射免疫以较低剂量保护了BALB/c小鼠。出乎意料的是,鼻内免疫的保护效果没有差异。尽管在CD46+转基因小鼠中恢复了Ad7的肌肉转导,但与BALB/c小鼠相比,抵抗流感攻击所需的剂量甚至更高。然而,与Ad4相比,经鼻内免疫的CD46+转基因小鼠得到了更好的保护。有趣的是,CD46+小鼠中Ad7转导的恢复并没有提高疫苗效力,这表明在没有CD46的情况下,Ad7可能通过替代受体转导不同的细胞亚群。这些数据表明,Ad4和Ad7都可以使用集中化的H1基因有效地诱导针对异源攻击的抗H1N1免疫力。未来在非人类灵长类动物中的研究或人体临床试验将确定Ad4和Ad7作为流感疫苗的总体有效性。

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