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Dietary Management of the Ketogenic Glycogen Storage Diseases

机译:生酮糖原贮积病的饮食管理

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The glycogen storage diseases (GSDs) comprise a group of rare inherited disorders of glycogen metabolism. The hepatic glycogenolytic forms of these disorders are typically associated with hypoglycemia and hepatomegaly. For GSD I, secondary metabolic disturbances include fasting hyperlactatemia, hyperuricemia, and hyperlipidemia. Glycogen storage disease III is caused by reduced activity of the debrancher enzyme, GSD VI by phosphorylase, and GSD IX by phosphorylase kinase. It has often been reported that the non-GSD I group of disorders have a benign course. However, myopathy, cardiomyopathy, and cirrhosis have been reported significant clinical morbidities associated with GSD III and IX in particular. There have been a range of reports indicating high-protein diets, high-fat diets, medium chain triglyceride (MCT), modified Atkins diet, and therapeutic ketones as rescuing severe phenotypes of GSD III in particular. The etiology of these severe phenotypes has not been defined. Cases presented in this report indicate potential harm from excessive simple sugar use in GSD IX C. Review of the literature indicates that most interventions have reduced the glycemic load and provide alternate substrates for energy in rescue situations. Prevention of complications is most likely to occur with a mixed balanced low glycemic index diet potentially with relative increases in protein.
机译:糖原贮积病(GSD)包括一组罕见的遗传性糖原代谢异常。这些疾病的肝糖原分解形式通常与低血糖症和肝肿大有关。对于GSD I,继发性代谢紊乱包括禁食高乳酸血症,高尿酸血症和高脂血症。糖原贮积病III是由脱支酶,磷酸化酶引起的GSD VI和磷酸化酶激酶引起的GSD IX活性降低引起的。经常有报道说,非GSD I类疾病具有良性病程。然而,据报道肌病,心肌病和肝硬化特别是与GSD III和IX相关的显着临床发病率。已有大量报道表明,高蛋白饮食,高脂饮食,中链甘油三酸酯(MCT),改良的阿特金斯饮食和治疗性酮尤其可挽救GSD III的严重表型。这些严重表型的病因尚未明确。本报告中的案例表明,GSD IX C中过量使用简单的糖有潜在的危害。文献回顾表明,大多数干预措施均降低了血糖负荷,并为救援提供了替代性的能量底物。混合均衡的低血糖指数饮食最有可能预防并发症,而蛋白质可能相对增加。

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