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首页> 外文期刊>Biomaterials >The effect of urine-derived stem cells expressing VEGF loaded in collagen hydrogels on myogenesis and innervation following after subcutaneous implantation in nude mice
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The effect of urine-derived stem cells expressing VEGF loaded in collagen hydrogels on myogenesis and innervation following after subcutaneous implantation in nude mice

机译:胶原水凝胶中载有表达VEGF的尿干细胞对裸鼠皮下植入后肌发生和神经支配的影响

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Impairment of sphincter muscles or their neural and vascular support leads to stress urinary incontinence. The aim of this study was to determine the role of urine-derived stem cells (USCs) over-expressing vascular endothelial growth factor (VEGF) in collagen-I gel on angiogenesis, cell survival, cell growth, myogenic phenotype differentiation of the implanted cells and innervations following implantation invivo. USCs were infected with adenovirus containing the human VEGF165 and green fluorescent protein genes. A total of 5×106 cells, USCs alone, or plus endothelial cells or human skeletal myoblasts (as control) suspended in collagen-I gel were subcutaneously implanted into nude mice. Extensive vascularization and more implanted cells was noted in VEGF-expressing USCs groups compared to the non-VEGF groups invivo. Numbers of the cells displaying endothelial markers (CD 31 and von Willebrand's factor) and myogenic markers (myf-5, MyoD and desmin), and regenerated nerve fibers displaying neural markers (S-100, GFAP and neurofilament) significantly increased in the grafts of VEGF-expressing USCs. Improved angiogenesis by VEGF-expressing USCs enhanced grafted cell survival, recruited the resident cells and promoted myogenic phenotype differentiation of USCs and innervation. This approach has important clinical implications for the development of cell therapies for the correction of stress urinary incontinence.
机译:括约肌或其神经和血管支持受损会导致压力性尿失禁。这项研究的目的是确定胶原蛋白-I凝胶中过表达尿干细胞(USCs)的血管内皮生长因子(VEGF)对血管生成,细胞存活,细胞生长,植入细胞的肌型表型分化的作用和植入体内后的神经支配。 USCs感染了包含人VEGF165和绿色荧光蛋白基因的腺病毒。将总共​​5×106个细胞,单独的USC或加上内皮细胞或人骨骼肌成肌细胞(作为对照)悬浮在I型胶原中,将其皮下植入裸鼠。与非VEGF组相比,在表达VEGF的USC组中发现了广泛的血管形成和更多的植入细胞。在移植的移植物中,内皮标记(CD 31和von Willebrand因子)和肌生标记(myf-5,MyoD和desmin)的细胞数和示神经标记(S-100,GFAP和神经丝)的再生神经纤维数量明显增加。表达VEGF的USC。通过表达VEGF的USC改善血管生成可提高移植细胞的存活率,募集驻留细胞并促进USC的肌型表型分化和神经支配。这种方法对纠正应激性尿失禁的细胞疗法的发展具有重要的临床意义。

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