Post-absorptive and insulin-mediated muscle protein metabolism in liver-transplanted patients
Autor: | L. Piceni Sereni, A. Pulvirenti, Vincenzo Mazzaferro, Livio Luzi, M. Spessot, D. Baratti, Enrico Regalia, Ileana Terruzzi, R. Romito |
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Rok vydání: | 2002 |
Předmět: |
Liver Cirrhosis
medicine.medical_specialty Phenylalanine Endocrinology Diabetes and Metabolism medicine.medical_treatment Protein metabolism Muscle Proteins Biology chemistry.chemical_compound Endocrinology Forearm Leucine Internal medicine medicine.artery Internal Medicine medicine Humans Insulin Glucose homeostasis Brachial artery Muscle Skeletal Skeletal muscle General Medicine Middle Aged Postprandial Period Liver Transplantation Transplantation medicine.anatomical_structure Liver chemistry Oxidation-Reduction Peptide Hydrolases |
Zdroj: | Acta Diabetologica. 39:203-208 |
ISSN: | 1432-5233 0940-5429 |
DOI: | 10.1007/s005920200035 |
Popis: | Cirrhotic patients after liver transplantation show a near-normal glucose homeostasis when in stable condition. In contrast, the basal and insulin-mediated whole-body protein metabolism remain altered several years after the graft. To examine whether the persisting defect of protein metabolism was due to the muscle, 7 non-diabetic liver-transplanted patients in stable condition were studied by means of the catheterization of the brachial artery and the deep forearm vein (to measure the balance across the forearm) and the infusion of labelled leucine and phenylalanine associated with indirect calorimetry. Whole-body proteolysis (as determined by endogenous leucine flux, ELF), protein synthesis (from non-oxidative leucine disposal, NOLD) and leucine oxidation (LO) were reduced in comparison to previously obtained values in a normal population. Insulin infusion (while maintaining euglycemia) induced a not significant variation of forearm phenylalanine Ra (24.4--16.5 micromol/100 ml forearm min(-1); proteolysis) and Rd (18.5--19.7; protein synthesis). In contrast, the whole-body insulin-dependent inhibitions of ELF (31.5--21.8 micromol/m(2) min) and NOLD (27.3--18.4) were impaired with respect to a normal population. On the basis of the present results, we conclude that skeletal muscle is not responsible for the alterations of leucine metabolism persisting after liver transplantation. By exclusion, this points to the liver as the major determinant of the leucine metabolism defect. |
Databáze: | OpenAIRE |
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