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狂犬病病毒发病机制与灭活和减毒狂犬病疫苗干预的关系。

Rabies virus pathogenesis in relationship to intervention with inactivated and attenuated rabies vaccines.

机构信息

Poxvirus and Rabies Branch, Division of Viral and Rickettsial Diseases, National Center for Zoonotic, Vector-borne and Enteric Diseases, Centers for Disease Control and Prevention, 1600 Clifton Road NE, Atlanta, GA 30333, USA.

出版信息

Vaccine. 2009 Nov 27;27(51):7149-55. doi: 10.1016/j.vaccine.2009.09.034.

Abstract

Despite progress in vaccine development in the past century the mechanisms behind immune responses elicited by rabies biologics or via natural infection remain largely unknown. In this study, we compared protection elicited by standard, early, or delayed prophylaxis with a reduced number of vaccine doses using inactivated and live-attenuated vaccines. Two-month-old Syrian hamsters, 4-week-old ICR mice or adult rhesus macaques were inoculated with canine rabies virus variants. Thereafter, prophylaxis was initiated 6h, 1, 2, 3, 4, 5, 6 or 7 days post-exposure (p.e.). One or several doses of inactivated (HDCV), or reverse genetically attenuated (live), or gamma-irradiated (inactivated)-ERAG333 vaccines were administered intramuscularly. The dynamics of virus spread were measured over time in the rodent models. Rabies virus reached the spinal cord at day 4 and brain at day 6 p.e. All hamsters succumbed in groups in which live ERAG333 was delayed until days 5 and 6 p.e. However, 78%, 44%, 56% and 22% of hamsters survived when one dose of live ERAG333 was administered 6h, 1, 2, 3, and 4 days p.e., respectively. Similarly, 67% survived when inactivated ERAG333 was administered at 24h p.e. All hamsters succumbed when standard prophylaxis (the Essen regimen) was delayed until days 3-6, but 67% and 33% of hamsters survived when PEP began 1 or 2 days p.e., respectively. Macaques were protected by one dose of attenuated ERAG333 at 24h p.e. The highly attenuated (live) and inactivated ERAG333 vaccines elicited potent protective immune responses, even when prophylaxis initiation was delayed. When 2-5 doses of commercial vaccine and HRIG were administered according to the Essen scheme, 89-100% of the animals survived. Reduced vaccine schedules provided efficacious intervention, regardless of the total number of vaccine doses administered.

摘要

尽管在过去一个世纪中疫苗研发取得了进展,但狂犬病生物制品或通过自然感染引发免疫反应的机制在很大程度上仍不清楚。在这项研究中,我们比较了使用减毒活疫苗和灭活疫苗,通过减少疫苗接种次数来进行标准、早期或延迟预防的保护效果。两个月大的叙利亚仓鼠、四周大的 ICR 小鼠或成年恒河猴用犬狂犬病病毒变异体接种。此后,在暴露后 6 小时、1 天、2 天、3 天、4 天、5 天、6 天或 7 天开始预防接种。通过肌肉内注射给予一剂或多剂减毒活(HDCV)或反向遗传减毒(活)或γ辐照(灭活)-ERAG333 疫苗。在啮齿动物模型中,随时间测量病毒传播的动态。狂犬病病毒在暴露后第 4 天到达脊髓,第 6 天到达大脑。所有的仓鼠都在延迟到第 5 天和第 6 天的活 ERAG333 组中死亡。然而,当在暴露后第 6 小时、第 1 天、第 2 天、第 3 天和第 4 天分别给予一剂活 ERAG333 时,78%、44%、56%和 22%的仓鼠存活。同样,在暴露后 24 小时给予灭活 ERAG333 时,67%的仓鼠存活。当标准预防接种(埃森方案)延迟到第 3-6 天时,所有的仓鼠都死亡,但当 PEP 在暴露后第 1 天或第 2 天开始时,67%和 33%的仓鼠存活。恒河猴在暴露后 24 小时给予一剂减毒 ERAG333 可得到保护。高度减毒(活)和灭活 ERAG333 疫苗即使在预防接种开始延迟的情况下也能引发有效的保护性免疫反应。当根据埃森方案给予 2-5 剂商业疫苗和 HRIG 时,89-100%的动物存活。无论给予的疫苗总剂量如何,减少疫苗接种次数均可提供有效的干预措施。

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