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Infection-enhancing lipopeptides do not improve intranasal immunization of cotton rats with a delta-G candidate live-attenuated human respiratory syncytial virus vaccine

机译:增强感染力的脂肽不能改善用delta-G候选减毒人类呼吸道合胞病毒疫苗对棉鼠的鼻内免疫

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摘要

textabstractDevelopment of live-attenuated human respiratory syncytial virus (HRSV) vaccines has proven to be difficult. Several vaccine candidates were found to be over-attenuated and displayed limited immunogenicity. Recently, we identified three synthetic cationic lipopeptides that enhanced paramyxovirus infections in vitro. The infection enhancement proved to be mediated by enhanced virus binding to target cells. We hypothesized that these lipopeptides can be used as adjuvants to promote immune responses induced by live-attenuated paramyxovirus vaccines. This hypothesis was tested in a vaccination and challenge model in cotton rats, using a previously described recombinant live-attenuated candidate HRSV vaccine lacking the gene encoding the G glycoprotein (rHRSVΔG). Surprisingly, intranasal vaccination of cotton rats with rHRSVΔG formulated in infection-enhancing lipopeptides resulted in reduced virus loads in nasopha-ryngeal lavages, reduced seroconversion levels and reduced protection from wild-type HRSV challenge. In conclusion, we were unable to demonstrate the feasibility of lipopeptides as adjuvants for a candidate live-attenuated HRSV vaccine in the cotton rat model.
机译:已证明开发减毒人类呼吸道合胞病毒(HRSV)疫苗是困难的。发现几种候选疫苗过度减毒并显示出有限的免疫原性。最近,我们确定了三种合成的阳离子脂肽,可增强体外副粘病毒感染。事实证明,感染增强是由病毒与靶细胞的结合增强所介导的。我们假设这些脂肽可以用作佐剂,以促进减毒副粘病毒活疫苗诱导的免疫反应。使用先前描述的缺乏编码G糖蛋白(rHRSVΔG)基因的重组减毒活HRSV候选疫苗,在棉鼠的疫苗接种和攻击模型中测试了该假设。出人意料的是,用增强感染的脂肽配制的rHRSVΔG对棉鼠进行鼻内疫苗接种可减少鼻咽-灌洗液中的病毒载量,降低血清转化水平,并减少对野生型HRSV攻击的保护。总之,我们无法证明脂肽作为棉鼠模型中候选减毒活SVSV疫苗佐剂的可行性。

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