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A novel endothelial cell-based gene therapy platform for the in vivo delivery of apolipoprotein E.

机译:一种新型的基于内皮细胞的基因治疗平台,用于体内载脂蛋白E。

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A major focus in gene therapy has been the use of recombinant viruses to deliver genes in vivo. Although this approach shows much promise, there are many safety concerns associated with the use of viral materials in the treatment of human diseases. Our alternative cell-based gene therapy approach utilizes endothelial cells (Pro 175) isolated from the murine embryonic yolk sac. These endothelial cells were evaluated for their potential use in gene therapy as a gene delivery platform. As a test model, we used these cells to deliver apolipoprotein E (apoE) in the murine apoE knockout atherosclerosis model. The lack of apoE protein in these animals results in high levels of serum cholesterol and formation of severe aortic plaques and lesions at a young age. After transplantation of the apoE secreting Pro 175 endothelial cells into apoE-deficient mice, serum cholesterol levels were measured at 2 week intervals. During the 3 months after the initiation of these experiments, levels of cholesterol in the animals having received the apoE secreting endothelial cells were statistically lower compared with the levels of age-matched controls having received non-secreting endothelial cells. Concomitant with cholesterol reduction, atherosclerotic aortic plaques were noticeably reduced in the experimental apoE+ animals. These results highlight the potential of these unique endothelial cells as an efficient delivery platform for somatic gene therapy.
机译:基因治疗的主要焦点是重组病毒在体内传递基因的使用。尽管这种方法显示出很大的希望,但在治疗人类疾病中使用病毒材料存在许多安全隐患。我们基于细胞的替代基因治疗方法利用从鼠卵黄囊分离的内皮细胞(Pro 175)。评价这些内皮细胞在基因治疗中作为基因传递平台的潜在用途。作为测试模型,我们使用这些细胞在鼠apoE敲除动脉粥样硬化模型中递送载脂蛋白E(apoE)。这些动物缺乏apoE蛋白会导致血清胆固醇水平升高,并在年轻时形成严重的主动脉斑块和病变。将分泌apoE的Pro 175内皮细胞移植到apoE缺陷型小鼠中后,每隔2周测量一次血清胆固醇水平。在这些实验开始后的3个月中,与年龄匹配的非分泌型内皮细胞对照相比,接受apoE分泌型内皮细胞的动物体内的胆固醇水平在统计学上较低。与胆固醇降低同时,实验性apoE +动物的动脉粥样硬化主动脉斑块明显减少。这些结果突出了这些独特的内皮细胞作为体细胞基因治疗的有效递送平台的潜力。

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