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Long-Term Efficacy and Safety of Insulin and Glucokinase Gene Therapy for Diabetes: 8-Year Follow-Up in Dogs

机译:胰岛素和葡糖激酶基因治疗糖尿病的长期疗效和安全性:狗的8年随访

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摘要

Diabetes is a complex metabolic disease that exposes patients to the deleterious effects of hyperglycemia on various organs. Achievement of normoglycemia with exogenous insulin treatment requires the use of high doses of hormone, which increases the risk of life-threatening hypoglycemic episodes. We developed a gene therapy approach to control diabetic hyperglycemia based on co-expression of the insulin and glucokinase genes in skeletal muscle. Previous studies proved the feasibility of gene delivery to large diabetic animals with adeno-associated viral (AAV) vectors. Here, we report the long-term (∼8 years) follow-up after a single administration of therapeutic vectors to diabetic dogs. Successful, multi-year control of glycemia was achieved without the need of supplementation with exogenous insulin. Metabolic correction was demonstrated through normalization of serum levels of fructosamine, triglycerides, and cholesterol and remarkable improvement in the response to an oral glucose challenge. The persistence of vector genomes and therapeutic transgene expression years after vector delivery was documented in multiple samples from treated muscles, which showed normal morphology. Thus, this study demonstrates the long-term efficacy and safety of insulin and glucokinase gene transfer in large animals and especially the ability of the system to respond to the changes in metabolic needs as animals grow older.
机译:糖尿病是一种复杂的代谢疾病,使患者容易遭受高血糖对各种器官的有害作用。通过外源性胰岛素治疗达到正常血糖需要使用大剂量激素,这会增加危及生命的降血糖事件的风险。我们基于骨骼肌中胰岛素和葡萄糖激酶基因的共表达,开发了一种基因治疗方法来控制糖尿病性高血糖症。先前的研究证明了使用腺相关病毒(AAV)载体将基因传递给大型糖尿病动物的可行性。在此,我们报告了对糖尿病犬单次使用治疗载体后的长期随访(约8年)。无需补充外源胰岛素即可成功实现多年的血糖控制。通过果糖胺,甘油三酸酯和胆固醇的血清水平正常化以及口服葡萄糖激发反应的显着改善,证明了代谢校正。载体递送后数年,载体基因组的持久性和治疗性转基因表达在来自治疗过的肌肉的多个样品中得到了证明,这些样品表现出正常的形态。因此,这项研究证明了胰岛素和葡萄糖激酶基因转移在大型动物中的长期疗效和安全性,尤其是随着动物年龄的增长,系统对代谢需求变化的反应能力。

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