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Recombinant adenovirus expressing ICP47 gene suppresses the ability of dendritic cells by restricting specific T cell responses

机译:表达ICP47基因的重组腺病毒通过限制特异性T细胞应答来抑制树突状细胞的能力

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Adenoviral vectors have been demonstrated to be one of the most effective vehicles to deliver foreign DNA into dendritic cells (DCs). However, the response of host immune systems against foreign gene products is a major obstacle to successful gene therapy. Infected cell protein 47 (ICP47) inhibits MHC [U+2160] antigen presentation pathway by binding to host transporter associated with antigen presentation (TAP), and thereby attenuates of specific cytotoxic T lymphocytes (CTLs) responses and evades the host immune clearance. This subject was designed to construct a recombinant adenovirus expressing His-tag-ICP47 fusion protein to investigate further the role of ICP47 in the elimination of transgene expression. Consequently, a recombinant adenovirus expressing the His-tag-ICP47 fusion protein was successfully constructed and it had the abilities of attenuating the stimulatory capacity of DCs by reducing the proliferation of lymphocytes and cytokine production of perforin compared with those of the r-track group and the control group. Our observations provide the first evidence of the regulation mechanism of ICP47 on DC-based immunotherapy for long-term persistence.
机译:腺病毒载体已被证明是将外源DNA输送至树突状细胞(DC)的最有效载体之一。但是,宿主免疫系统对外源基因产物的反应是成功进行基因治疗的主要障碍。感染的细胞蛋白47(ICP47)通过与与抗原呈递(TAP)相关的宿主转运蛋白结合来抑制MHC [U + 2160]抗原呈递途径,从而减弱特定的细胞毒性T淋巴细胞(CTL)反应并逃避宿主的免疫清除。设计该受试者以构建表达His-tag-ICP47融合蛋白的重组腺病毒,以进一步研究ICP47在消除转基因表达中的作用。因此,成功构建了表达His-tag-ICP47融合蛋白的重组腺病毒,与r-track组相比,它具有通过减少淋巴细胞的增殖和穿孔素的细胞因子产生而减弱DCs的刺激能力的能力。对照组。我们的观察结果提供了ICP47对基于DC的免疫治疗的长期持久性调控机制的第一个证据。

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