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Effect of targeted ovarian cancer therapy using amniotic fluid mesenchymal stem cells transfected with enhanced green fluorescent protein-human interleukin-2 in vivo

机译:转染增强型绿色荧光蛋白-人白介素2的羊水间充质干细胞在体内靶向卵巢癌的治疗效果

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摘要

The aim of the present study was to investigate the effect of using amniotic fluid mesenchymal stem cells (AF-MSCs) in targeted ovarian cancer therapy in vivo. AF-MSCs were isolated from human second trimester AF and a plasmid, enhanced green fluorescent protein-human interleukin-2 (pEGFP-hIL-2) was formed. The plasmid was stably transfected into the AF-MSCs and the cells were intravenously injected into ovarian cancer nude mice models. Following stable transfection of the vector, tumor formation, and the expression and activity of hIL-2 were investigated, and microscopic pathological examinations of the tumor were performed. It was found that AF-MSCs exhibited high motility during migration in vivo, and the vector, pEGFP-hIL-2 can be stably transfected into AF-MSCs. Following stable transfection, this type of stem cell is able to successfully transport the therapeutic gene, IL-2, migrate to the ovarian cancer tumor site to secrete the functional IL-2 and treat the tumor. Thus, AF-MSCs may serve as transporters for therapeutic genes targeting ovarian tumor sites and, therefore, be involved in the treatment of tumors.
机译:本研究的目的是研究在体内靶向卵巢癌治疗中使用羊水间充质干细胞(AF-MSC)的效果。从人的中期妊娠AF中分离AF-MSC,并形成质粒,形成增强的绿色荧光蛋白-人白介素2(pEGFP-hIL-2)。将该质粒稳定转染到AF-MSC中,并将细胞静脉内注射到卵巢癌裸鼠模型中。稳定转染载体后,研究了肿瘤的形成以及hIL-2的表达和活性,并对肿瘤进行了显微病理检查。发现AF-MSC在体内迁移过程中表现出高的运动性,并且载体pEGFP-hIL-2可以被稳定地转染到AF-MSC中。稳定转染后,这种类型的干细胞能够成功转运治疗性基因IL-2,迁移至卵巢癌肿瘤部位以分泌功能性IL-2并治疗肿瘤。因此,AF-MSC可以充当靶向卵巢肿瘤位点的治疗基因的转运蛋白,因此参与肿瘤的治疗。

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