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Adenoviral vector-mediated insulin gene transfer in the mouse pancreas corrects streptozotocin-induced hyperglycemia.

机译:腺病毒载体介导的胰岛素基因在小鼠胰腺中的转移可纠正链脲佐菌素诱导的高血糖症。

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摘要

Therapy for type 1 diabetes consists of tight blood glucose (BG) control to minimize complications. Current treatment relies on multiple insulin injections or an insulin pump placement, beta-cell or whole pancreas transplantation. All approaches have significant limitations and have led to the realization that novel treatment strategies are needed. Pancreatic acinar cells have features that make them a good target for insulin gene transfer. They are not subject to autoimmune attack, a problem with pancreas or islets transplantation, they are avidly transduced by recombinant adenoviral vectors, and capable of exporting a variety of peptides into the portal circulation. Recombinant adenoviral vectors were engineered to express either wild-type or furin-modified human insulin cDNA (AdCMVhInsM). Immunodeficient mice were made diabetic with streptozotocin and injected intrapancreatically with the vectors. BG and blood insulin levels have normalized after administration of AdCMVhInsM. Immunohistochemistry and electron microscopy showed the presence of insulin in acinar cells throughout the pancreas and localization of insulin molecules to acinar cell vesicles. The data clearly establish a relationship between intrapancreatic vector administration, decreased BG and elevated blood insulin levels. The findings support the use of pancreatic acinar cells to express and secrete insulin into the blood stream.
机译:1型糖尿病的治疗包括严格控制血糖(BG),以最大程度地减少并发症。当前的治疗依赖于多次胰岛素注射或胰岛素泵植入,β细胞或全胰腺移植。所有方法都有明显的局限性,并导致认识到需要新颖的治疗策略。胰腺腺泡细胞具有使其成为胰岛素基因转移的良好靶标的功能。它们不受自身免疫攻击,胰腺或胰岛移植问题的困扰,可以通过重组腺病毒载体进行狂热转导,并且能够将多种肽输出到门脉循环中。重组腺病毒载体经工程改造以表达野生型或弗林蛋白酶修饰的人胰岛素cDNA(AdCMVhInsM)。用链脲佐菌素使免疫不足的小鼠患糖尿病,并用载体胰内注射。服用AdCMVhInsM后,BG和血液胰岛素水平已恢复正常。免疫组织化学和电子显微镜检查显示,整个胰腺的腺泡细胞中都存在胰岛素,并且胰岛素分子位于腺泡囊泡中。数据清楚地建立了胰腺内载体给药,BG降低和血液胰岛素水平升高之间的关系。这些发现支持使用胰腺腺泡细胞在血液中表达和分泌胰岛素。

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