首页> 外文期刊>Journal of Controlled Release: Official Journal of the Controlled Release Society >Adenovirus serotype 35 vector-induced innate immune responses in dendritic cells derived from wild-type and human CD46-transgenic mice: Comparison with a fiber-substituted Ad vector containing fiber proteins of Ad serotype 35
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Adenovirus serotype 35 vector-induced innate immune responses in dendritic cells derived from wild-type and human CD46-transgenic mice: Comparison with a fiber-substituted Ad vector containing fiber proteins of Ad serotype 35

机译:腺病毒血清型35载体诱导的野生型和人CD46转基因小鼠树突状细胞的先天免疫应答:与含有Ad血清型35纤维蛋白的纤维取代的Ad载体的比较

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摘要

Recently, much attention has focused on replication-incompetent adenovirus (Ad) vectors containing fiber proteins derived from species B Ad serotype 35 (Ad35) (Ad5F35) and Ad vectors fully constructed from Ad35 as vaccine vectors expressing antigens. However, differences in the transduction properties, including the induction of innate immunity, of Ad5F35 and Ad35 vectors have not been properly and fully examined, partly because the transduction properties of these Ad vectors should be evaluated using nonhuman primates or human CD46-transgenic (CD46TG) mice, which ubiquitously express the primary receptor of Ad35, human CD46, in a pattern similar to that of humans. In the present study, we evaluated innate immune responses of mouse dendritic cells (mDCs) derived from bone marrow cells of wild-type (WT) and CD46TG mice following transduction with Ad serotype 5 (Ad5), fiber-substituted Ad5F35, or Ad35 vectors. Ad5F35 and Ad35 vectors mediated more efficient transduction in mDCs derived from CD46TG mice (CD46TG-mDCs) than did Ad5 vectors. Upregulation of costimulatory molecules and inflammatory cytokine induction by Ad5F35 and Ad35 vectors were significantly higher than those by Ad5 vectors in CD46TG-mDCs. However, the induction properties of the innate immune responses were different between Ad5F35 and Ad35 vectors. Ad35 vectors induced higher levels of costimulatory molecule expression and inflammatory cytokine production than did Ad5F35 vectors in CD46TG-mDCs. Furthermore, intravenous administration of Ad35 vectors in WT and CD46TG mice resulted in higher levels of serum interleukin (IL)-6 and IL-12 compared with administration of Ad5F35 vectors, which exhibited almost mock-transduced levels of these inflammatory cytokines. This study indicates that innate immune responses by Ad35 and Ad5F35 vectors are distinct even although both Ad vectors recognize human CD46 as a receptor.
机译:近来,许多注意力集中在不能复制的腺病毒(Ad)载体上,该载体含有衍生自物种B Ad血清型35(Ad35)(Ad5F35)的纤维蛋白,和完全由Ad35构建的Ad载体作为表达抗原的疫苗载体。但是,尚未对Ad5F35和Ad35载体的转导特性(包括先天免疫的诱导)进行差异性和充分检查,部分原因是应使用非人类灵长类动物或人类CD46转基因(CD46TG)评估这些Ad载体的转导特性。 )小鼠,其以与人相似的模式普遍表达Ad35的主要受体,即人CD46。在本研究中,我们评估了Ad血清型5(Ad5),纤维取代的Ad5F35或Ad35载体转导后,源自野生型(WT)和CD46TG小鼠骨髓细胞的小鼠树突状细胞(mDC)的先天免疫应答。与Ad5载体相比,Ad5F35和Ad35载体在CD46TG小鼠(CD46TG-mDCs)衍生的mDC中介导的转导效率更高。在CD46TG-mDC中,Ad5F35和Ad35载体对共刺激分子的上调和炎症细胞因子的诱导显着高于Ad5载体。但是,先天免疫应答的诱导特性在Ad5F35和Ad35载体之间是不同的。与CD46TG-mDC中的Ad5F35载体相比,Ad35载体诱导了更高水平的共刺激分子表达和炎性细胞因子产生。此外,与施用Ad5F35载体相比,在WT和CD46TG小鼠中静脉内施用Ad35载体导致较高的血清白介素(IL)-6和IL-12水平,所述Ad5F35载体表现出这些炎性细胞因子几乎是模拟转导的水平。这项研究表明,尽管两个Ad载体都将人CD46识别为受体,但Ad35和Ad5F35载体的先天免疫应答却截然不同。

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