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Muscle stem cells can act as antigen-presenting cells: implication for gene therapy.

机译:肌肉干细胞可以充当抗原呈递细胞:对基因疗法的意义。

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Research has shown that the use of a muscle-specific promoter can reduce immune response and improve gene transfer to muscle fibers. We investigated the efficiency of direct and ex vivo gene transfer to the skeletal muscles of 6- to 8-week-old mdx mice by using two adenoviral vectors: adenovirus (AD) encoding the luciferase gene under the cytomegalovirus (CMV) promoter (ADCMV) and AD encoding the same gene under the muscle creatine kinase (MCK) promoter (ADMCK). Direct intramuscular injection of ADMCK triggered a lower immune response that enabled more efficient delivery and more persistent expression of the transgene than did ADCMV injection. Similarly, ex vivo gene transfer using ADCMV-transduced muscle-derived stem cells (MDSCs) induced a stronger immune response and led to shorter transgene expression than did ex vivo gene transfer using ADMCK-transduced MDSCs. This immune response was due to the release of the antigen after MDSC death or to the ADCMV-transduced MDSCs acting as antigen-presenting cells (APCs) by expressing the transgene and rapidly initiating an immune response against subsequent viral inoculation. The use of a muscle-specific promoter that restricts transgene expression to differentiated muscle cells could prevent MDSCs from becoming APCs, and thereby could improve the efficiency of ex vivo gene transfer to skeletal muscle.
机译:研究表明,使用特定于肌肉的启动子可以减少免疫反应并改善基因向肌肉纤维的转移。我们研究了通过使用两种腺病毒载体将直接和离体基因转移到6至8周龄mdx小鼠骨骼肌的效率:在巨细胞病毒(CMV)启动子(ADCMV)下编码荧光素酶基因的腺病毒(AD)和AD在肌肉肌酸激酶(MCK)启动子(ADMCK)下编码相同的基因。与ADCMV注射相比,直接肌内注射ADMCK触发了较低的免疫反应,从而使转基因的传递效率更高,表达更持久。类似地,与使用ADMCK转导的MDSC进行离体基因转移相比,使用ADCMV转导的肌肉衍生干细胞(MDSC)进行离体基因转移诱导了更强的免疫反应,并导致较短的转基因表达。这种免疫应答是由于MDSC死亡后抗原的释放,或归因于ADCMV转导的MDSC通过表达转基因并迅速启动针对随后病毒接种的免疫应答而充当抗原呈递细胞(APC)。使用将转基因表达限制在分化的肌肉细胞中的肌肉特异性启动子可以防止MDSC成为APC,从而可以提高离体基因转移到骨骼肌的效率。

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