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 inInternational Journal of Obesity Vol. 24; no. 10; pp. 1297 - 1302
Main Authors Paquot, N, Schneiter, P, Scheen, A.J, Lefebvre, P.J, Tappy, L
Format Journal Article Web Resource
LanguageEnglish
Published England Nature Publishing Group 01.10.2000
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ISSN0307-0565
1476-5497
1476-5497
DOI10.1038/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.
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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BackLink https://www.ncbi.nlm.nih.gov/pubmed/11093291$$D View this record in MEDLINE/PubMed
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CitedBy_id crossref_primary_10_1002_mas_20021
crossref_primary_10_1016_j_nut_2006_04_004
crossref_primary_10_1016_S0014_2999_02_02726_7
Cites_doi 10.1093/ajcn/51.4.571
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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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