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首页> 外文期刊>The Journal of Infectious Diseases >Intradermal Vaccination With Adjuvanted Ebola Virus Soluble Glycoprotein Subunit Vaccine by Microneedle Patches Protects Mice Against Lethal Ebola Virus Challenge
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Intradermal Vaccination With Adjuvanted Ebola Virus Soluble Glycoprotein Subunit Vaccine by Microneedle Patches Protects Mice Against Lethal Ebola Virus Challenge

机译:用微针贴片与辅助埃博拉病毒可溶性糖蛋白亚基疫苗的皮内接种疫苗保护小鼠免受致死的埃博拉病毒攻击

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摘要

In this study, we investigated immune responses induced by purified Ebola virus (EBOV) soluble glycoprotein (sGP) subunit vaccines via intradermal immunization with microneedle (MN) patches in comparison with intramuscular (IM) injection in mice. Our results showed that MN delivery of EBOV sGP was superior to IM injection in eliciting higher levels and longer lasting antibody responses against EBOV sGP and GP antigens. Moreover, sGP-specific immune responses induced by MN or IM immunizations were effectively augmented by formulating sGP with a saponin-based adjuvant, and they were shown to confer complete protection of mice against lethal mouse-adapted EBOV (MA-EBOV) challenge. In comparison, mice that received sGP without adjuvant by MN or IM immunizations succumbed to lethal MA-EBOV challenge. These results show that immunization with EBOV sGP subunit vaccines with adjuvant by MN patches, which have been shown to provide improved safety and thermal stability, is a promising approach to protect against EBOV infection.
机译:在该研究中,我们通过与微小(IM)注射在小鼠中,通过用微针(Mn)贴片,通过皮内免疫进行纯化的埃博拉病毒(EBOV)可溶性糖蛋白(SGP)亚基疫苗诱导的免疫应答。我们的研究结果表明,EBOV SGP的MN递送优于ENM注射,以引出较高水平和持久抗体反应对EBOV SGP和GP抗原的持久性反应。此外,通过用皂苷类佐剂配制SGP有效地增强了由Mn或IM免疫引起的SGP特异性免疫应答,并且显示它们对致死的小鼠适应的EBOV(MA-EBOV)攻击进行完全保护小鼠。相比之下,接受SGP的小鼠没有通过Mn或IM免疫求助于致命的Ma-Ebov挑战。这些结果表明,通过Mn贴片与EBOV SGP亚基疫苗免疫,已被证明提供改善的安全性和热稳定性,是一种有希望的防止EBOV感染的方法。

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