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Melanoma Cell Viability is Reduced after Endoglin Silencing with Gene Electrotransfer

机译:在用基因电转换器沉默后,黑色素瘤细胞活力降低

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Tumor angiogenesis represents a promising target for cancer treatment. Tumor endothelial cells proliferate faster than normal endothelial cells due to activation of specific endothelial cell markers. One of them is endoglin, a Transforming Growth Factor p (TGF-p") co-receptor, involved predominantly in cellular proliferation and migration. Besides the expression of endoglin in tumor endothelial cells, it is also expressed in some types of tumor cells, especially in melanoma. Therefore, in melanoma, targeting endoglin could provide a beneficial therapeutic effect based on simultaneously inhibiting angiogenesis and melanoma cell proliferation. Therefore, the aim of our study was to determine the level of endoglin expression in endothelial and tumor cell lines (melanoma and adenocarcinoma) and to investigate if endoglin expression is associated with changes in cell viability after endoglin silencing. Our study showed that endothelial and melanoma cells express high levels of endoglin and that after endoglin silencing with gene electrotranfer (GET), cell viability was specifically decreased, whereas in tumor cells with low expression of endoglin, only non-specific decrease in cell viability was observed after GET. Our study is one of the first studies exploring the effect of endoglin on biological properties of melanoma cells and indicates new possibilities for melanoma treatment with targeted gene therapy approach.
机译:肿瘤血管生成代表癌症治疗的有希望的靶标。由于特定内皮细胞标记物的激活,肿瘤内皮细胞比正常内皮细胞更快地增殖。其中一个是indoglan,一种转化的生长因子p(TGF-p“)共同受体,主要涉及细胞增殖和迁移。除了肿瘤内皮细胞中的胚胎林的表达外,还在某些类型的肿瘤细胞中表达,特别是黑色素瘤。因此,在黑色素瘤中,靶向胚胎林可以基于同时抑制血管生成和黑素瘤细胞增殖提供有益的治疗效果。因此,我们的研究目的是确定内皮和肿瘤细胞系中的内阴光表达水平(黑色素瘤和腺癌)和探讨内阴光蛋白表达与内烟嘴沉默后的细胞活力的变化相关。我们的研究表明,内皮和黑素瘤细胞表达了高水平的内核林,并且在用基因电替替替替替替替替者(GET)沉默后,细胞活力明确降低,而在肿瘤细胞中具有低表达的胚胎蛋白,但仅在细胞空间中的非特异性降低在得到后观察到。我们的研究是探讨内切胶类对黑素瘤细胞生物学性质的第一研究之一,并表明了具有靶向基因治疗方法的黑色素瘤治疗的新可能性。

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