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Improving the Safety of a Conditional-Live Human Immunodeficiency Virus Type 1 Vaccine by Controlling both Gene Expression and Cell Entry

机译:通过控制基因表达和细胞进入来提高有条件生活的人类免疫缺陷病毒1型疫苗的安全性

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摘要

Live attenuated human immunodeficiency virus type 1 (HIV-1) vaccines are considered unsafe because faster-replicating pathogenic virus variants may evolve after vaccination. We previously presented a conditional-live HIV-1 variant of which replication can be switched off as an alternative vaccination strategy. To improve the safety of such a vaccine, we constructed a new HIV-1 variant that depends not only on doxycycline for gene expression but also on the T20 peptide for cell entry. Replication of this virus can be limited to the level required to induce the immune system by transient administration of doxycycline and T20. Subsequent withdrawal of these inducers efficiently blocks viral replication and evolution.
机译:减毒的1型人类免疫缺陷病毒活疫苗被认为是不安全的,因为在疫苗接种后可能会进化出更快复制的病原病毒变体。我们先前介绍过一种条件活的HIV-1变体,可以将其复制作为替代疫苗接种策略。为了提高这种疫苗的安全性,我们构建了一个新的HIV-1变体,该变体不仅依赖强力霉素进行基因表达,而且依赖T20肽进入细胞。该病毒的复制可以限制在通过强力霉素和T20的瞬时给药来诱导免疫系统所需的水平上。随后撤回这些诱导物可有效阻断病毒复制和进化。

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