The Dietary Treatment of Children with Type I Glycogen Storage Disease with Slow Release Carbohydrate

Abstract: SummaryThe effect of ingestion of uncooked cornstarch (2 g/kg body weight) in water, uncooked starch (1 g/kg) added to a meal, and glucose (2 g/kg) in water, was studied in eight patients with type IA glycogen storage disease (GSD) and one patient with type IB GSD. Blood glucose concentrations were determined at 30-min intervals during each tolerance test; blood lactate, blood insulin, and expiratory hydrogen were determined at 60-min intervals. The glucose levels remained in the normal range (L1.8 mM) during … Show more

“…Later, uncooked corn starch was used to replace nocturnal intragastric drip feeding since glucose is slowly released and absorbed from this low-glycaemicindex food, so that normoglycaemia may be maintained for 6-8 h [3]. However, in many patients on uncooked corn starch ideal plasma glucose concentrations are not achieved and hyperlactataemia occurred after midnight [5,11,15,17,18]. Since it could not be excluded that the poor metabolic control would impair growth and allow formation of hepatic adenomas with malignant potential, we refused to treat our patients with nocturnal uncooked corn starch during childhood.…”

Type I glycogen storage disease: favourable outcome on a strict management regimen avoiding increased lactate production during childhood and adolescence

“…Later, uncooked corn starch was used to replace nocturnal intragastric drip feeding since glucose is slowly released and absorbed from this low-glycaemicindex food, so that normoglycaemia may be maintained for 6-8 h [3]. However, in many patients on uncooked corn starch ideal plasma glucose concentrations are not achieved and hyperlactataemia occurred after midnight [5,11,15,17,18]. Since it could not be excluded that the poor metabolic control would impair growth and allow formation of hepatic adenomas with malignant potential, we refused to treat our patients with nocturnal uncooked corn starch during childhood.…”

Type I glycogen storage disease: favourable outcome on a strict management regimen avoiding increased lactate production during childhood and adolescence

“…Clinical pathology includes profound enlargement of the liver and kidneys because of excess glycogen accumulation, and shunting into alternative pathways results in hyperlipidemia, hyperuricemia, and lactic acidosis (Chen and Burchell, 1995;Chou et al, 2002;Wolfsdorf et al, 2003). Current therapy is palliative, with the aim of controlling hypoglycemia by providing continuous sources of glucose via frequent feedings, continuous overnight feeding by nasogastric tube, and/or oral administration of uncooked cornstarch or other starches (Chen et al, 1984;Smit et al, 1984Smit et al, , 1988Fernandes et al, 1988;Bhattacharya et al, 2007). Affected patients can now survive to adulthood, but long-term complications remain common, including hepatic adenomas, hepatocellular carcinoma, renal disease, gout, osteoporosis, and pulmonary hypertension (Smit et al, 1990;Mundy et al, 2003Mundy et al, , 2005Ozen, 2007).…”

Adeno-Associated Virus-Mediated Correction of a Canine Model of Glycogen Storage Disease Type Ia

“…Provision of exogenous glucose to GSD I patients has altered over the years [1,6,7,11,12,15,26,36,37,45,46]. Methods are frequent feedings, meals and snacks preferably with precooked cornstarch (PCCS), continuous nocturnal gastric drip feeding (CNGDF) and administration of uncooked cornstarch (UCSS).…”

Guidelines for management of glycogen storage disease type I - European Study on Glycogen Storage Disease Type I (ESGSD I)