Role of Glucagon in Catabolism and Muscle Wasting of Critical Illness and Modulation by Nutrition

Role of Glucagon in Catabolism and Muscle Wasting of Critical Illness and Modulation by Nutrition

Critical illness is hallmarked by muscle wasting and disturbances in glucose, lipid, and amino acid homeostasis. Circulating concentrations of glucagon, a catabolic hormone that affects these metabolic pathways, are elevated during critical illness. Insight in the nutritional regulation of glucagon...

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Veröffentlicht in:American journal of respiratory and critical care medicine 2017-11, Vol.196 (9), p.1131-1143
Hauptverfasser: Thiessen, Steven E, Derde, Sarah, Derese, Inge, Dufour, Thomas, Vega, Chloé Albert, Langouche, Lies, Goossens, Chloë, Peersman, Nele, Vermeersch, Pieter, Vander Perre, Sarah, Holst, Jens J, Wouters, Pieter J, Vanhorebeek, Ilse, Van den Berghe, Greet
Format: Artikel
Sprache:eng
Schlagworte:
Aged
Amino acids
Amino Acids - blood
Animals
Blood Glucose
Critical Illness
Diabetes
Disease Models, Animal
Female
Glucagon - blood
Glucagon - metabolism
Glucose
Glucose - administration & dosage
Growth factors
Homeostasis
Humans
Hyperglycemia
Illnesses
Insulin
Insulin - administration & dosage
Insulin - blood
Intensive care
Lipids
Male
Metabolism
Mice
Middle Aged
Muscular Atrophy - blood
Muscular Atrophy - metabolism
Muscular Atrophy - therapy
Nutrition
Parenteral nutrition
Parenteral Nutrition - methods
Plasma
Rodents
Sepsis
Treatment Outcome
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Zusammenfassung:Critical illness is hallmarked by muscle wasting and disturbances in glucose, lipid, and amino acid homeostasis. Circulating concentrations of glucagon, a catabolic hormone that affects these metabolic pathways, are elevated during critical illness. Insight in the nutritional regulation of glucagon and its metabolic role during critical illness is lacking. To evaluate whether macronutrient infusion can suppress plasma glucagon during critical illness and study the role of illness-induced glucagon abundance in the disturbed glucose, lipid, and amino acid homeostasis and in muscle wasting during critical illness. In human and mouse studies, we infused macronutrients and manipulated glucagon availability up and down to investigate its acute and chronic metabolic role during critical illness. In critically ill patients, infusing glucose with insulin did not lower glucagon, whereas parenteral nutrition containing amino acids increased glucagon. In critically ill mice, infusion of amino acids increased glucagon and up-regulated markers of hepatic amino acid catabolism without affecting muscle wasting. Immunoneutralizing glucagon in critically ill mice only transiently affected glucose and lipid metabolism, did not affect muscle wasting, but drastically suppressed markers of hepatic amino acid catabolism and reversed the illness-induced hypoaminoacidemia. These data suggest that elevated glucagon availability during critical illness increases hepatic amino acid catabolism, explaining the illness-induced hypoaminoacidemia, without affecting muscle wasting and without a sustained impact on blood glucose. Furthermore, amino acid infusion likely results in a further breakdown of amino acids in the liver, mediated by increased glucagon, without preventing muscle wasting. Clinical trial registered with www.clinicaltrials.gov (NCT 00512122).
ISSN:1073-449X
1535-4970
DOI:10.1164/rccm.201702-0354OC