Assessment of postprandial hepatic glycogen synthesis from uridine diphosphoglucose kinetics in obese and lean non-diabetic subjects
BACKGROUND: Obese patients are frequently characterized by insulin resistance and decreased insulin-mediated glycogen synthesis in skeletal muscle. Whether they also have impaired postprandial hepatic glycogen synthesis remains unknown. AIM: To determine whether postprandial hepatic glycogen synthes...
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Published in | International Journal of Obesity Vol. 24; no. 10; pp. 1297 - 1302 |
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Main Authors | , , , , |
Format | Journal Article Web Resource |
Language | English |
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England
Nature Publishing Group
01.10.2000
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ISSN | 0307-0565 1476-5497 1476-5497 |
DOI | 10.1038/sj.ijo.0801386 |
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Abstract | BACKGROUND: Obese patients are frequently characterized by insulin resistance and decreased insulin-mediated glycogen synthesis in skeletal muscle. Whether they also have impaired postprandial hepatic glycogen synthesis remains unknown. AIM: To determine whether postprandial hepatic glycogen synthesis is decreased in obese patients compared to lean subjects. METHODS: Lean and obese subjects with impaired glucose tolerance were studied over 4 h after ingestion of a glucose load. Hepatic uridine diphosphoglucose kinetics were assessed using 13C-galactose infusion, with monitoring of urinary acetaminophen-glucuronide isotopic enrichment to estimate hepatic glycogen kinetics. RESULTS: Estimated net hepatic glycogen synthesis amounted to 18.6 and 22.6% of the ingested load in lean and obese subjects, respectively. CONCLUSION: Postprandial hepatic glycogen metabolism is not impaired in non-diabetic obese subjects. |
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AbstractList | BACKGROUND: Obese patients are frequently characterized by insulin resistance and decreased insulin-mediated glycogen synthesis in skeletal muscle. Whether they also have impaired postprandial hepatic glycogen synthesis remains unknown. AIM: To determine whether postprandial hepatic glycogen synthesis is decreased in obese patients compared to lean subjects. METHODS: Lean and obese subjects with impaired glucose tolerance were studied over 4h after ingestion of a glucose load. Hepatic uridine diphosphoglucose kinetics were assessed using 13C-galactose infusion, with monitoring of urinary acetaminophen-glucuronide isotopic enrichment to estimate hepatic glycogen kinetics. RESULTS: Estimated net hepatic glycogen synthesis amounted to 18.6 and 22.6% of the ingested load in lean and obese subjects, respectively. CONCLUSION: Postprandial hepatic glycogen metabolism is not impaired in non-diabetic obese subjects. Obese patients are frequently characterized by insulin resistance and decreased insulin-mediated glycogen synthesis in skeletal muscle. Whether they also have impaired postprandial hepatic glycogen synthesis remains unknown. To determine whether postprandial hepatic glycogen synthesis is decreased in obese patients compared to lean subjects. Lean and obese subjects with impaired glucose tolerance were studied over 4h after ingestion of a glucose load. Hepatic uridine diphosphoglucose kinetics were assessed using 13C-galactose infusion, with monitoring of urinary acetaminophen-glucuronide isotopic enrichment to estimate hepatic glycogen kinetics. Estimated net hepatic glycogen synthesis amounted to 18.6 and 22.6% of the ingested load in lean and obese subjects, respectively. Postprandial hepatic glycogen metabolism is not impaired in non-diabetic obese subjects. BACKGROUND: Obese patients are frequently characterized by insulin resistance and decreased insulin-mediated glycogen synthesis in skeletal muscle. Whether they also have impaired postprandial hepatic glycogen synthesis remains unknown. AIM: To determine whether postprandial hepatic glycogen synthesis is decreased in obese patients compared to lean subjects. METHODS: Lean and obese subjects with impaired glucose tolerance were studied over 4 h after ingestion of a glucose load. Hepatic uridine diphosphoglucose kinetics were assessed using 13 C-galactose infusion, with monitoring of urinary acetaminophen-glucuronide isotopic enrichment to estimate hepatic glycogen kinetics. RESULTS: Estimated net hepatic glycogen synthesis amounted to 18.6 and 22.6% of the ingested load in lean and obese subjects, respectively. CONCLUSION: Postprandial hepatic glycogen metabolism is not impaired in non-diabetic obese subjects. International Journal of Obesity (2000) 24, 1297-1302 BACKGROUND: Obese patients are frequently characterized by insulin resistance and decreased insulin-mediated glycogen synthesis in skeletal muscle. Whether they also have impaired postprandial hepatic glycogen synthesis remains unknown. AIM: To determine whether postprandial hepatic glycogen synthesis is decreased in obese patients compared to lean subjects. METHODS: Lean and obese subjects with impaired glucose tolerance were studied over 4 h after ingestion of a glucose load. Hepatic uridine diphosphoglucose kinetics were assessed using 13C-galactose infusion, with monitoring of urinary acetaminophen-glucuronide isotopic enrichment to estimate hepatic glycogen kinetics. RESULTS: Estimated net hepatic glycogen synthesis amounted to 18.6 and 22.6% of the ingested load in lean and obese subjects, respectively. CONCLUSION: Postprandial hepatic glycogen metabolism is not impaired in non-diabetic obese subjects. |
Author | Tappy, L Lefebvre, P.J Scheen, A.J Paquot, N Schneiter, P |
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Cites_doi | 10.1093/ajcn/51.4.571 10.1016/S0950-351X(05)80207-1 10.1172/JCI115997 10.1016/0026-0495(88)90129-1 10.1002/dmr.5610030107 10.1046/j.1365-2362.1999.00003.x 10.2337/diab.44.9.1038 10.1016/S0026-0495(97)90137-2 10.2337/diacare.21.1.S5 10.1172/JCI117913 10.1172/JCI117602 10.1172/JCI118379 10.1079/BJN19740060 10.2337/diab.46.2.204 10.1016/S0026-0495(99)90265-2 10.2337/diab.39.11.1381 10.1056/NEJM199001253220403 10.1056/NEJM199201023260104 10.1007/s001250050141 10.2337/diabetes.48.5.1198 10.1073/pnas.85.13.4682 |
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References | P Schneiter (BF0801386_CR21) 1999; 48 DS Gray (BF0801386_CR15) 1990; 51 JE Gerich (BF0801386_CR2) 1993; 7 PJ Lefèbvre (BF0801386_CR1) 1999; 29 G Shulman (BF0801386_CR11) 1990; 322 B Ludvik (BF0801386_CR12) 1995; 95 R DeBodo (BF0801386_CR18) 1963; 19 JP Felber (BF0801386_CR10) 1992 A. D. Cherrington (BF0801386_CR7) 1999; 48 I Magnusson (BF0801386_CR17) 1988; 85 AJ Scheen (BF0801386_CR25) 1995; 19 K Rebrin (BF0801386_CR4) 1995; 44 BF0801386_CR20 MK Hellerstein (BF0801386_CR19) 1997; 46 L Tappy (BF0801386_CR3) 1995; 21 W Stalmans (BF0801386_CR5) 1987; 3 I Magnusson (BF0801386_CR22) 1992; 90 GW Cline (BF0801386_CR24) 1994; 94 MK Hellerstein (BF0801386_CR13) 1988; 37 A Mitrakou (BF0801386_CR9) 1992; 326 LJ Gay (BF0801386_CR16) 1994; 37 R Taylor (BF0801386_CR23) 1996; 97 L Tappy (BF0801386_CR6) 1997; 46 JVGA Durnin (BF0801386_CR14) 1979; 32 A Mitrakou (BF0801386_CR8) 1990; 39 |
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Snippet | BACKGROUND: Obese patients are frequently characterized by insulin resistance and decreased insulin-mediated glycogen synthesis in skeletal muscle. Whether... Obese patients are frequently characterized by insulin resistance and decreased insulin-mediated glycogen synthesis in skeletal muscle. Whether they also have... |
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SubjectTerms | Adult Aged Analgesics analysis biosynthesis blood Blood Glucose Blood Glucose - analysis Carbohydrates complications Diabetes Endocrinologie, métabolisme & nutrition Endocrinology, metabolism & nutrition Fatty Acids, Nonesterified Fatty Acids, Nonesterified - blood Female Glucose Glucose Intolerance Glucose Intolerance - complications Glucose Intolerance - metabolism Glucose Intolerance/complications/metabolism glucose tolerance glycogen Homeostasis Human health sciences Humans Hyperglycemia Ingestion Insulin Insulin - blood Insulin Resistance Isotopic enrichment Kinetics Liver Liver - metabolism Liver Glycogen Liver Glycogen - biosynthesis Male metabolic diseases Metabolism Middle Aged monitoring Musculoskeletal system Obesity Obesity - complications Obesity - metabolism Obesity/complications/metabolism patients pharmacokinetics Physiology Postprandial Period Sciences de la santé humaine skeletal muscle Time Factors uridine Uridine Diphosphate Glucose Uridine Diphosphate Glucose - metabolism Uridine Diphosphate Glucose - pharmacokinetics Uridine Diphosphate Glucose/metabolism/pharmacokinetics |
Title | Assessment of postprandial hepatic glycogen synthesis from uridine diphosphoglucose kinetics in obese and lean non-diabetic subjects |
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