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Efficient gene delivery to pancreatic islets with ultrasonic microbubble destruction technology

机译:超声微泡破坏技术有效地将基因传递到胰岛

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摘要

This study describes a method of gene delivery to pancreatic islets of adult, living animals by ultrasound targeted microbubble destruction (UTMD). The technique involves incorporation of plasmids into the phospholipid shell of gas-filled microbubbles, which are then infused into rats and destroyed within the pancreatic microcirculation with ultrasound. Specific delivery of genes to islet beta cells by UTMD was achieved by using a plasmid containing a rat insulin 1 promoter (RIP), and reporter gene expression was regulated appropriately by glucose in animals that received a RIP–luciferase plasmid. To demonstrate biological efficacy, we used UTMD to deliver RIP–human insulin and RIP–hexokinase I plasmids to islets of adult rats. Delivery of the former plasmid resulted in clear increases in circulating human C-peptide and decreased blood glucose levels, whereas delivery of the latter plasmid resulted in a clear increase in hexokinase I protein expression in islets, increased insulin levels in blood, and decreased circulating glucose levels. We conclude that UTMD allows relatively noninvasive delivery of genes to pancreatic islets with an efficiency sufficient to modulate beta cell function in adult animals.
机译:这项研究描述了通过超声靶向微泡破坏(UTMD)将基因传递到成年活体胰腺胰岛的方法。该技术涉及将质粒掺入充气微泡的磷脂壳中,然后将其注入大鼠体内并在超声作用下破坏胰腺微循环。通过使用含有大鼠胰岛素1启动子(RIP)的质粒,可以通过UTMD将基因特异性地转运至胰岛β细胞,并且在接受RIP-荧光素酶质粒的动物体内,葡萄糖适当地调节了报告基因的表达。为了证明其生物学功效,我们使用UTMD将RIP-人胰岛素和RIP-己糖激酶I质粒递送给成年大鼠的胰岛。前一种质粒的递送导致循环的人C肽明显增加并降低血糖水平,而后一种质粒的递送导致胰岛中的己糖激酶I蛋白表达明显增加,血液中胰岛素水平增加和循环葡萄糖降低水平。我们得出结论,UTMD允许相对无创地将基因传递给胰岛,其效率足以调节成年动物的β细胞功能。

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