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Abstract
Severe malnutrition accounts for half-a-million deaths annually in children under the age of five. Despite improved WHO guidelines, inpatient mortality remains high and is associated with metabolic dysfunction. Previous studies suggest a correlation between hepatic metabolic dysfunction and impaired autophagy. We aimed to determine the role of mTORC1 inhibition in a murine model of malnutrition-induced hepatic dysfunction. Wild type weanling C57/B6 mice were fed a 18 or 1% protein diet for two weeks. A third low-protein group received daily rapamycin injections, an mTORC1 inhibitor. Hepatic metabolic function was assessed by histology, immunofluorescence, gene expression, metabolomics and protein levels. Low protein-fed mice manifested characteristics of severe malnutrition, including weight loss, hypoalbuminemia, hypoglycemia, hepatic steatosis and cholestasis. Low protein-fed mice had fewer mitochondria and showed signs of impaired mitochondrial function. Rapamycin prevented hepatic steatosis, restored ATP levels and fasted plasma glucose levels compared to untreated mice. This correlated with increased content of LC3-II, and decreased content mitochondrial damage marker, PINK1. We demonstrate that hepatic steatosis and disturbed mitochondrial function in a murine model of severe malnutrition can be partially prevented through inhibition of mTORC1. These findings suggest that stimulation of autophagy could be a novel approach to improve metabolic function in severely malnourished children.
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Details
1 Hospital for Sick Children, Translational Medicine Program, Toronto, Canada (GRID:grid.42327.30) (ISNI:0000 0004 0473 9646); University Medical Center Groningen, Department of Pediatrics, Section of Molecular Metabolism and Nutrition, Groningen, The Netherlands (GRID:grid.4494.d) (ISNI:0000 0000 9558 4598)
2 Hospital for Sick Children, Translational Medicine Program, Toronto, Canada (GRID:grid.42327.30) (ISNI:0000 0004 0473 9646)
3 Hospital for Sick Children, Translational Medicine Program, Toronto, Canada (GRID:grid.42327.30) (ISNI:0000 0004 0473 9646); The Childhood Acute Illness and Nutrition Network, Nairobi, Kenya (GRID:grid.511677.3)
4 University of Toronto, Department of Biochemistry, Faculty of Medicine, Toronto, Canada (GRID:grid.17063.33) (ISNI:0000 0001 2157 2938); Hospital for Sick Children, Cell Biology Program, Toronto, Canada (GRID:grid.42327.30) (ISNI:0000 0004 0473 9646)
5 University Medical Center Groningen, Department of Pediatrics, Section of Molecular Metabolism and Nutrition, Groningen, The Netherlands (GRID:grid.4494.d) (ISNI:0000 0000 9558 4598)
6 Hospital for Sick Children, Translational Medicine Program, Toronto, Canada (GRID:grid.42327.30) (ISNI:0000 0004 0473 9646); University of Toronto, Department of Nutritional Sciences, Faculty of Medicine, Toronto, Canada (GRID:grid.17063.33) (ISNI:0000 0001 2157 2938)
7 Hospital for Sick Children, Translational Medicine Program, Toronto, Canada (GRID:grid.42327.30) (ISNI:0000 0004 0473 9646); University Medical Center Groningen, Department of Pediatrics, Section of Molecular Metabolism and Nutrition, Groningen, The Netherlands (GRID:grid.4494.d) (ISNI:0000 0000 9558 4598); The Childhood Acute Illness and Nutrition Network, Nairobi, Kenya (GRID:grid.511677.3); University of Toronto, Department of Nutritional Sciences, Faculty of Medicine, Toronto, Canada (GRID:grid.17063.33) (ISNI:0000 0001 2157 2938); University of Toronto, Department of Biochemistry, Faculty of Medicine, Toronto, Canada (GRID:grid.17063.33) (ISNI:0000 0001 2157 2938); Hospital for Sick Children, Centre for Global Child Health, Toronto, Canada (GRID:grid.42327.30) (ISNI:0000 0004 0473 9646)