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首页> 外文期刊>Molecular therapy: the journal of the American Society of Gene Therapy >A critical role for type I IFN-dependent NK cell activation in innate immune elimination of adenoviral vectors in vivo.
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A critical role for type I IFN-dependent NK cell activation in innate immune elimination of adenoviral vectors in vivo.

机译:I型IFN依赖性NK细胞激活在体内先天免疫消除腺病毒载体中的关键作用。

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摘要

Recombinant adenoviruses have been used widely for gene therapy due to their high transduction efficiency in vivo. However, the attendant innate immune response to adenoviral vectors has limited their applications for in vivo gene therapy. Recent studies have shown that adenoviruses activate the innate immunity through both Toll-like receptor-dependent (TLR-dependent) and TLR-independent pathways, leading to the production of type I interferons (IFNs) and other inflammatory cytokines. Furthermore, type I IFNs play a pivotal role in innate immune elimination of adenoviral vectors in vivo. It remains to be defined how type I IFNs regulate innate immune clearance of adenoviral vectors. In this study, we showed in vivo that natural killer (NK) cells were activated and accumulated in the liver upon intravenous administration of adenoviral vectors, leading to the loss of adenoviral genome and the reduction of transgene expression. We further demonstrated that type I IFNs were critical for the activation of NK cells. This was achieved by direct action of type I IFNs on NK cells. Overall, our observations reveal a critical role for type I IFN-dependent NK cell activation in innate immune elimination of adenoviral vectors in vivo and may help design effective strategies to improve the outcome of adenovirus-mediated gene therapy.
机译:重组腺病毒由于其体内高转导效率而被广泛用于基因治疗。但是,伴随的对腺病毒载体的先天免疫应答限制了它们在体内基因治疗中的应用。最近的研究表明,腺病毒通过Toll样受体依赖性(TLR依赖性)和TLR依赖性途径激活先天免疫,从而导致产生I型干扰素(IFN)和其他炎性细胞因子。此外,I型IFN在体内先天免疫消除腺病毒载体中起关键作用。 I型IFN如何调节腺病毒载体的先天免疫清除尚待确定。在这项研究中,我们在体内显示,通过静脉内注射腺病毒载体,自然杀伤(NK)细胞被激活并在肝脏中积累,从而导致腺病毒基因组丢失和转基因表达降低。我们进一步证明,I型干扰素对于激活NK细胞至关重要。这是通过I型IFN对NK细胞的直接作用来实现的。总体而言,我们的观察结果揭示了I型IFN依赖性NK细胞激活在体内先天免疫体内消除腺病毒载体中的关键作用,并且可能有助于设计有效的策略来改善腺病毒介导的基因治疗的结果。

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