首页> 外文期刊>Molecular therapy: the journal of the American Society of Gene Therapy >Toll-like receptor 9 triggers an innate immune response to helper-dependent adenoviral vectors.
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Toll-like receptor 9 triggers an innate immune response to helper-dependent adenoviral vectors.

机译:Toll样受体9触发对辅助依赖型腺病毒载体的先天免疫应答。

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摘要

A major obstacle to the clinical application of systemic adenoviral gene replacement therapy is the host innate immune response. Although recent studies have attempted to characterize the cellular basis for this response to systemically administered helper-dependent adenoviral vector (HD-Ad), the underlying molecular components of the innate immune repertoire required to recognize the viral vector have yet to be identified. Here, we show that primary macrophages can sense HD-Ad vectors via the Toll-like Receptor 9 (TLR9) and respond by increasing pro-inflammatory cytokine secretion. Moreover, TLR9 sensing is involved in the rapid innate immune response to HD-Ad in vivo. TLR9 deficiency attenuates the innate immune response to HD-Ad, whereas TLR9 blockade reduces the acute inflammatory response after intravenous injection of the vector. Moreover, HD-Ad upregulates TLR9 gene expression independent of TLR9 function, suggesting that additional innate signaling pathways work cooperatively with TLR9. The identification of the components of the innate immune response to adenovirus will facilitate the development of combinatorial therapy directed at increasing the maximal tolerated dose of systemically delivered adenoviral vectors.
机译:全身性腺病毒基因替代疗法的临床应用的主要障碍是宿主固有免疫反应。尽管最近的研究试图表征对全身给药的依赖于辅助物的腺病毒载体(HD-Ad)的这种反应的细胞基础,但尚未确定识别病毒载体所需的先天免疫库的潜在分子成分。在这里,我们显示初级巨噬细胞可以通过Toll样受体9(TLR9)感知HD-Ad载体,并通过增加促炎性细胞因子的分泌来做出反应。此外,TLR9感应涉及体内对HD-Ad的快速先天免疫应答。 TLR9缺乏症减弱了对HD-Ad的先天免疫反应,而TLR9阻断作用减少了静脉内注射载体后的急性炎症反应。此外,HD-Ad上调了TLR9基因表达,而与TLR9功能无关,这表明其他先天信号通路与TLR9协同工作。对腺病毒的先天免疫应答的成分的鉴定将促进针对增加全身递送的腺病毒载体的最大耐受剂量的组合疗法的发展。

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