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A novel Chimpanzee serotype-based adenoviral vector as delivery tool for cancer vaccines

机译:基于黑猩猩血清型的新型腺病毒载体作为癌症疫苗的递送工具

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摘要

The use of adenovirus (Ad) as vaccine vectors is hindered by pre-existing immunity to human Ads in most of the human population. In order to overcome this limitation, uncommon alternative Ad serotypes need to be utilized. In this study, an E1-E3 deleted recombinant Ad based on the chimpanzee serotype 3 (ChAd3) was engineered to express human carcinoembryonic antigen (CEA) protein or rat neu extracellular/transmembrane domains (ECD.TM). ChAd3 vectors were tested in CEA transgenic (CEA.Tg) and BALB/NeuT mice, which show immunologic tolerance to these antigens. ChAd3 is capable of inducing an immune response comparable to that of hAd5 serotype-based vectors, thus breaking tolerance to tumor associated antigens (TAAs) and achieving anti-tumor effects. Of importance is that ChAd3 can overcome hAd5 pre-existing immunity and work in conjunction with DNA electroporation (DNA-EP) and other Ad vaccines based on common human serotypes.
机译:腺病毒(Ad)作为疫苗载体的使用受到大多数人中预先存在的对人类Ad的免疫力的阻碍。为了克服此限制,需要使用不常见的替代Ad血清型。在这项研究中,基于黑猩猩血清型3(ChAd3)的E1-E3缺失重组Ad被工程化以表达人癌胚抗原(CEA)蛋白或大鼠神经元胞外/跨膜结构域(ECD.TM)。 ChAd3载体在CEA转基因(CEA.Tg)和BALB / NeuT小鼠中进行了测试,它们显示出对这些抗原的免疫耐受性。 ChAd3能够诱导与基于hAd5血清型的载体相当的免疫反应,从而打破了对肿瘤相关抗原(TAA)的耐受性并实现了抗肿瘤作用。重要的是ChAd3可以克服hAd5先前存在的免疫力,并与DNA电穿孔(DNA-EP)和其他基于普通人类血清型的Ad疫苗结合使用。

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