College of Veterinary Medicine, North Carolina State University, Raleigh, NC, USA.
Gene Ther. 2012 Apr;19(4):443-52. doi: 10.1038/gt.2011.86. Epub 2011 Jun 9.
Glycogen storage disease type Ia (GSD-Ia) stems from glucose-6-phosphatase (G6Pase) deficiency and causes hypoglycemia, hepatomegaly, hypercholesterolemia and lactic acidemia. Three dogs with GSD-Ia were initially treated with a helper-dependent adenovirus encoding a human G6Pase transgene (HDAd-cG6Pase serotype 5) on postnatal day 3. Unlike untreated dogs with GSD-Ia, all three dogs initially maintained normal blood glucose levels. After 6-22 months, vector-treated dogs developed hypoglycemia, anorexia and lethargy, suggesting that the HDAd-cG6Pase serotype 5 vector had lost efficacy. Liver biopsies collected at this time revealed significantly elevated hepatic G6Pase activity and reduced glycogen content, when compared with affected dogs treated only by frequent feeding. Subsequently, the HDAd-cG6Pase serotype 2 vector was administered to two dogs, and hypoglycemia was reversed; however, renal dysfunction and recurrent hypoglycemia complicated their management. Administration of a serotype 2 HDAd vector prolonged survival in one GSD-Ia dog to 12 months of age and 36 months of age in the other, but the persistence of long-term complications limited HDAd vectors in the canine model for GSD-Ia.
糖原贮积病 Ia 型(GSD-Ia)源于葡萄糖-6-磷酸酶(G6Pase)缺乏,导致低血糖、肝肿大、高胆固醇血症和乳酸性酸中毒。三只 GSD-Ia 犬在出生后第 3 天接受了编码人 G6Pase 转基因的辅助依赖性腺病毒(HDAd-cG6Pase 血清型 5)治疗。与未经治疗的 GSD-Ia 犬不同,所有三只犬最初均维持正常血糖水平。6-22 个月后,接受载体治疗的犬出现低血糖、食欲不振和昏睡,表明 HDAd-cG6Pase 血清型 5 载体已失去疗效。此时采集的肝活检显示,与仅通过频繁喂养治疗的受影响犬相比,肝 G6Pase 活性显著升高,糖原含量降低。随后,给两只犬施用了 HDAd-cG6Pase 血清型 2 载体,低血糖得到纠正;然而,肾功能障碍和反复低血糖使它们的治疗复杂化。血清型 2 HDAd 载体的给药将一只 GSD-Ia 犬的存活期延长至 12 个月,另一只延长至 36 个月,但长期并发症的持续存在限制了 HDAd 载体在犬 GSD-Ia 模型中的应用。
