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Sertoli Cells Engineered to Express Insulin to Lower Blood Glucose in Diabetic Mice

机译:塞托罗里细胞工程化以表达胰岛素在糖尿病小鼠中降低血糖

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Long-term survival of allo- and xenotransplanted immune-privileged Sertoli cells (SCs) is well documented suggesting that SCs can be used to deliver foreign proteins for cell-based gene therapy. The aim of this study was to use a lentivirus carrying proinsulin cDNA to achieve stable expression and lowering of blood glucose levels (BGLs). A SC line transduced with the lentivirus (MSC-LV-mI) maintained stable insulin expression in vitro. These MSC-LV-mI cells were transplanted and grafts were analyzed for cell survival, continued proinsulin mRNA, and insulin protein expression. All grafts contained MSC-LV-mI cells that expressed proinsulin mRNA and insulin protein. Transplantation of MSC-LV-mI cells into diabetic mice significantly lowered BGLs for 4 days after transplantation. Interestingly, in three transplanted SCID mice and one transplanted BALB/c mouse, the BGLs again significantly lowered by day 50 and 70, respectively. This is the first time SC transduced with a lentiviral vector was able to stably express insulin and lower BGLs. In conclusion, a SC line can be modified to stably express therapeutic proteins (e.g., insulin), thus taking us one step further in the use of SCs as an immune-privileged vehicle for cell-based gene therapy.
机译:丙二醇和异种包体的免疫特征的长期存活率良好地记录了SCS,表明SC可用于递送基于细胞的基因疗法的外蛋白。本研究的目的是使用携带慢病毒的携带胰岛素cDNA来实现稳定的表达和降低血糖水平(BGL)。用慢病毒(MSC-LV-MI)转导的SC线在体外维持稳定的胰岛素表达。将这些MSC-LV-MI细胞移植,分析移植物,用于细胞存活,继续的胰岛素mRNA和胰岛素蛋白表达。所有移植物含有表达胰岛素mRNA和胰岛素蛋白的MSC-LV-MI细胞。移植后4天,将MSC-LV-MI细胞移植到糖尿病小鼠中明显降低了BGL。有趣的是,在三个移植的SCID小鼠和一个移植的BALB / C小鼠中,BGL分别在第50和70天分别显着降低。这是用慢病毒载体转导的第一次能够稳定地表达胰岛素和低谷BGL。总之,可以修饰SC线以稳定表达治疗蛋白(例如,胰岛素),从而在使用SCS作为基于细胞基因疗法的免疫特权载体中进一步服用一步。

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