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首页> 外文期刊>Clinical and vaccine immunology: CVI >Attenuation of Replication-Competent Adenovirus Serotype 26 Vaccines by Vectorization
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Attenuation of Replication-Competent Adenovirus Serotype 26 Vaccines by Vectorization

机译:通过矢量化衰减复制能力的腺病毒血清型26疫苗

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Replication-competent adenovirus (rcAd)-based vaccine vectors may theoretically provide immunological advantages over replication- incompetent Ad vectors, but they also raise additional potential clinical and regulatory issues. We produced replication-competent Ad serotype 26 (rcAd26) vectors by adding the E1 region back into a replication-incompetent Ad26 vector backbone with the E3 or E3/E4 regions deleted. We assessed the effect of vectorization on the replicative capacity of the rcAd26 vaccines. Attenuation occurred in a stepwise fashion, with E3 deletion, E4 deletion, and human immunodeficiency virus type 1 (HIV-1) envelope (Env) gene insertion all contributing to reduced replicative capacity compared to that with the wild-type Ad26 vector. The rcAd26 vector with E3 and E4 deleted and containing the Env transgene exhibited 2.7- to 4.4-log-lower replicative capacity than that of the wild-type Ad26 in vitro. This rcAd26 vector is currently being evaluated in a phase 1 clinical trial. Attenuation as a result of vectorization and transgene insertion has implications for the clinical development of replication-competent vaccine vectors.
机译:基于复制功能的腺病毒(RCAD)基于基于复制的疫苗可能在理论上可以提供免疫学的优势,而不是复制 - 无能的AD载体,但它们也引发了额外的潜在临床和调节问题。我们通过将E1区域添加回具有E3或E3/E4区域的E1型AD26矢量主链中,从而产生了具有复制功能的AD血清型26(RCAD26)向量。我们评估了矢量化对RCAD26疫苗复制能力的影响。衰减以逐步的方式发生,具有E3缺失,E4缺失和人类免疫缺陷病毒1型(HIV-1)信封(ENV)基因插入,所有这些基因插入均与野生型AD26载体相比有助于降低复制能力。具有E3和E4的RCAD26载体已删除并包含ENV转基因的RCAD26载体表现出2.7至4.4-Log的复制能力,而不是体外的野生型AD26。该RCAD26矢量目前正在1期临床试验中进行评估。载体和转基因插入导致的衰减对复制能力疫苗载体的临床发展有影响。

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