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Improvements in gene therapy technologies.

机译:基因治疗技术的改进。

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We have combined hemagglutinating virus of Japan (HVJ; Sendai virus) with liposomes for efficient in vitro and in vivo fusion-mediated gene delivery. The HVJ-liposome was a highly efficient vehicle for the introduction of oligonucleotides into cells in vivo as well as for the transfer of genes <100 kbp without damaging cells. By coupling the Epstein-Barr (EB) virus replicon apparatus with HVJ-liposomes (virosomes), transgene expression was sustained in vitro and in vivo. When we added cationic lipids, the HVJ-cationic liposomes increased gene delivery 100 to 800 times in vitro compared with the conventional anionic virosomes and were also more useful for gene expression in restricted areas of organs and for gene therapy of disseminated cancers. We further discovered that the use of anionic virosomes with a virus-mimicking lipid composition (artificial viral envelope; AVE type) increased transfection efficiency approximately 10 fold in vivo, especially in the heart, liver, kidney, and muscle. Most animal organs were found to be suitable targets for the fusigenic virosomes, and numerous gene therapy strategies using this system were successful in animals. The combination of suicide gene therapy with radiation was very effective for killing hepatomas in a mouse model. Arteriosclerosis obliterans in animal models was cured by the transfer of hepatocyte growth factor.
机译:我们将日本的血凝病毒(HVJ;仙台病毒)与脂质体结合在一起,以有效地进行体外和体内融合介导的基因传递。 HVJ脂质体是一种高效的载体,可将寡核苷酸体内引入细胞,以及在不损伤细胞的情况下转移<100 kbp的基因。通过将爱泼斯坦-巴尔(EB)病毒复制子设备与HVJ-脂质体(病毒体)偶联,可在体内和体外维持转基因表达。当我们添加阳离子脂质时,与常规的阴离子病毒体相比,HVJ阳离子脂质体在体外的基因传递增加了100到800倍,并且对于器官有限区域的基因表达和散发性癌症的基因治疗也更有用。我们进一步发现,将阴离子病毒体与模拟病毒的脂质组合物(人工病毒包膜; AVE型)一起使用,可以提高体内大约10倍的转染效率,尤其是在心脏,肝脏,肾脏和肌肉中。发现大多数动物器官是融合型病毒体的合适靶标,并且使用该系统的许多基因治疗策略在动物中都是成功的。自杀基因疗法与放射疗法的结合对杀死小鼠模型中的肝癌非常有效。动物模型中的闭塞性动脉硬化症通过肝细胞生长因子的转移而治愈。

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