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首页> 外文期刊>Journal of Infectious Diseases >Replication-Deficient Rabies Virus–Based Vaccines Are Safe and Immunogenic in Mice and Nonhuman Primates
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Replication-Deficient Rabies Virus–Based Vaccines Are Safe and Immunogenic in Mice and Nonhuman Primates

机译:基于复制缺陷狂犬病病毒的疫苗在小鼠和非人类灵长类动物中安全且具有免疫原性

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摘要

Although current postexposure prophylaxis rabies virus (RV) vaccines are effective, ∼40,000–70,000 rabies-related deaths are reported annually worldwide. The development of effective formulations requiring only 1–2 applications would significantly reduce mortality. We assessed in mice and nonhuman primates the efficacy of replication-deficient RV vaccine vectors that lack either the matrix (M) or phosphoprotein (P) gene. A single dose of M gene–deficient RV induced a more rapid and efficient anti-RV response than did P gene–deficient RV immunization. Furthermore, the M gene–deleted RV vaccine induced 4-fold higher virus-neutralizing antibody (VNA) levels in rhesus macaques than did a commercial vaccine within 10 days after inoculation, and at 180 days after immunization rhesus macaques remained healthy and had higher-avidity antibodies, higher VNA titers, and a more potent antibody response typical of a type 1 T helper response than did animals immunized with a commercial vaccine. The data presented in this article suggest that the M gene–deleted RV vaccine is safe and effective and holds the potential of replacing current pre- and postexposure RV vaccines
机译:尽管目前的暴露后预防狂犬病病毒疫苗是有效的,但全世界每年据报有约40,000至70,000例狂犬病相关死亡。开发仅需要1-2次施用的有效制剂将大大降低死亡率。我们在小鼠和非人类灵长类动物中评估了缺乏基质(M)或磷蛋白(P)基因的复制缺陷型RV疫苗载体的功效。与缺乏P基因的RV免疫相比,单剂量的M基因缺陷的RV诱导更快,更有效的抗RV反应。此外,缺失M基因的RV疫苗在接种后10天内和免疫后180天内,猕猴的病毒中和抗体(VNA)水平比市售疫苗高4倍,而恒河猴保持健康并具有更高的-亲和力抗体,更高的VNA滴度以及比用市售疫苗免疫的动物更强的典型1型T辅助反应的抗体反应。本文提供的数据表明,缺失M基因的RV疫苗是安全有效的,并具有替代当前暴露前和暴露后RV疫苗的潜力

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