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首页> 外文期刊>Scientific reports. >Intradermal immunization by Ebola virus GP subunit vaccines using microneedle patches protects mice against lethal EBOV challenge
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Intradermal immunization by Ebola virus GP subunit vaccines using microneedle patches protects mice against lethal EBOV challenge

机译:埃博拉病毒GP亚基免疫接种使用微针贴片保护小鼠免受致死的EBOV挑战

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摘要

Development of a safe and efficacious filovirus vaccine is of high importance to public health. In this study, we compared immune responses induced by Ebola virus (EBOV) glycoprotein (GP) subunit vaccines via intradermal immunization with microneedle (MN) patches and the conventional intramuscular (IM) injection in mice, which showed that MN delivery of GP induced higher levels and longer lasting antibody responses against GP than IM injection. Further, we found that EBOV GP in formulation with a saponin-based adjuvant, Matrix-M, can be efficiently loaded onto MN patches. Co-delivery of Matrix-M with GP significantly enhanced induction of antibody responses by MN delivery, as also observed for IM injection. Results from challenge studies showed that all mice that received the GP/adjuvant formulation by MN or IM immunizations were protected from lethal EBOV challenge. Further, 4 out of 5 mice vaccinated by MN delivery of unadjuvanted GP also survived the challenge, whereas only 1 out of 5 mice vaccinated by IM injection of unadjuvanted GP survived the challenge. These results demonstrate that MN patch delivery of EBOV GP subunit vaccines, which is expected to enable improved safety and thermal stability, can confer effective protection against EBOV infection that is superior to IM vaccination.
机译:开发安全和有效的泌尿病疫苗对公共卫生具有很高的重要性。在本研究中,我们将埃博拉病毒(EBOV)糖蛋白(GP)亚基(GP)亚基疫苗诱导的免疫应答通过用微针(Mn)贴片和常规肌肉内(IM)注射在小鼠中,表明MN递送GP诱导水平和更长的抗体对GP的反应而不是Im注射。此外,我们发现,通过基于Saponin的佐剂,基质-M的配制中的EBOV GP可以有效地装载到Mn贴片上。与GP的基质-M的共递送显着增强了Mn递送的抗体应答的诱导,如IM注射的。挑战性研究的结果表明,受到Mn或IM免疫接种的所有小鼠免疫接受免疫致死。此外,由Mn递送的未破坏GP疫苗的5只小鼠中的4只也存在于挑战中,而仅通过IM注射未经调节的GP疫苗的5只小鼠中的1个幸存下来。这些结果表明,EBOV GP亚基疫苗的Mn贴剂递送,预期能够改善安全性和热稳定性,可以有效地保护EBOV感染,其优于IM疫苗接种。

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