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首页> 外文期刊>Gene therapy >Increased interstitial pressure improves nucleic acid delivery to skin enabling a comparative analysis of constitutive promoters.
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Increased interstitial pressure improves nucleic acid delivery to skin enabling a comparative analysis of constitutive promoters.

机译:升高的组织间隙压力改善了向皮肤的核酸递送,从而能够对组成型启动子进行比较分析。

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摘要

Nucleic acid-based therapies hold great promise for treatment of skin disorders if delivery challenges can be overcome. To investigate one mechanism of nucleic acid delivery to keratinocytes, a fixed mass of expression plasmid was intradermally injected into mouse footpads in different volumes, and reporter expression was monitored by intravital imaging or skin sectioning. Reporter gene expression increased with higher delivery volumes, suggesting that pressure drives nucleic acid uptake into cells after intradermal injections similar to previously published studies for muscle and liver. For spatiotemporal analysis of reporter gene expression, a dual-axis confocal (DAC) fluorescence microscope was used for intravital imaging following intradermal injections. Individual keratinocytes expressing hMGFP were readily visualized in vivo and initially appeared to preferentially express in the stratum granulosum and subsequently migrate to the stratum corneum over time. Fluorescence microscopy of frozen skin sections confirmed the patterns observed by intravital imaging. Intravital imaging with the DAC microscope is a noninvasive method for probing spatiotemporal control of gene expression and should facilitate development and testing of new nucleic acid delivery technologies.
机译:如果可以克服传递难题,则基于核酸的疗法有望治疗皮肤疾病。为了研究将核酸递送至角质形成细胞的一种机制,将固定质量的表达质粒皮内注射到不同体积的小鼠足垫中,并通过活体成像或皮肤切片监测报告基因的表达。报告基因的表达随输送量的增加而增加,表明皮内注射后压力驱动核酸吸收进入细胞,类似于先前发表的有关肌肉和肝脏的研究。为了对报告基因的表达进行时空分析,皮内注射后使用双轴共聚焦(DAC)荧光显微镜进行活体成像。表达hMGFP的单个角质形成细胞易于在体内观察到,最初似乎优先在颗粒层中表达,随后随时间迁移到角质层。冷冻皮肤切片的荧光显微镜检查证实了通过活体成像观察到的模式。用DAC显微镜进行活体成像是探测基因表达时空控制的一种非侵入性方法,应有助于开发和测试新的核酸递送技术。

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