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超声响应型甘露糖修饰基因载体的构建及其用于 DNA 疫苗治疗。

Development of an ultrasound-responsive and mannose-modified gene carrier for DNA vaccine therapy.

机构信息

Department of Drug Delivery Research, Graduate School of Pharmaceutical Sciences, Kyoto University, Sakyo-ku, Kyoto, Japan.

出版信息

Biomaterials. 2010 Oct;31(30):7813-26. doi: 10.1016/j.biomaterials.2010.06.058. Epub 2010 Jul 24.

DOI:10.1016/j.biomaterials.2010.06.058
PMID:20656348
Abstract

Development of a gene delivery system to transfer the gene of interest selectively and efficiently into targeted cells is essential for achievement of sufficient therapeutic effects by gene therapy. Here, we succeeded in developing the gene transfection method using ultrasound (US)-responsive and mannose-modified gene carriers, named Man-PEG(2000) bubble lipoplexes. Compared with the conventional lipofection method using mannose-modified carriers, this transfection method using Man-PEG(2000) bubble lipoplexes and US exposure enabled approximately 500-800-fold higher gene expressions in the antigen presenting cells (APCs) selectively in vivo. This enhanced gene expression was contributed by the improvement of delivering efficiency of nucleic acids to the targeted organs, and by the increase of introducing efficiency of nucleic acids into the cytoplasm followed by US exposure. Moreover, high anti-tumor effects were demonstrated by applying this method to DNA vaccine therapy using ovalbumin (OVA)-expressing plasmid DNA (pDNA). This US-responsive and cell-specific gene delivery system can be widely applied to medical treatments such as vaccine therapy and anti-inflammation therapy, which its targeted cells are APCs, and our findings may help in establishing innovative methods for in-vivo gene delivery to overcome the poor introducing efficiency of carriers into cytoplasm which the major obstacle associated with gene delivery by non-viral carriers.

摘要

开发一种基因传递系统,将目的基因选择性和有效地传递到靶细胞中,对于基因治疗达到足够的治疗效果是至关重要的。在这里,我们成功地开发了一种使用超声(US)响应和甘露糖修饰的基因载体的基因转染方法,命名为 Man-PEG(2000) 泡囊脂质体。与使用甘露糖修饰载体的常规转染方法相比,这种使用 Man-PEG(2000) 泡囊脂质体和 US 暴露的转染方法可使抗原呈递细胞(APCs)中约 500-800 倍的基因表达更高。这种增强的基因表达是由于提高了核酸向靶器官的传递效率,以及 US 暴露后增加了核酸进入细胞质的引入效率。此外,通过将该方法应用于含有卵清蛋白(OVA)表达质粒 DNA(pDNA)的 DNA 疫苗治疗,显示出了高抗肿瘤效果。这种 US 响应和细胞特异性基因传递系统可广泛应用于疫苗治疗和抗炎治疗等医学治疗,其靶细胞为 APCs,我们的发现可能有助于建立创新的体内基因传递方法,以克服非病毒载体基因传递中载体进入细胞质的引入效率差这一主要障碍。

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Development of an ultrasound-responsive and mannose-modified gene carrier for DNA vaccine therapy.超声响应型甘露糖修饰基因载体的构建及其用于 DNA 疫苗治疗。
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