Different Mechanisms for Impaired Fasting Glucose and Impaired Postprandial Glucose Tolerance in Humans
- 1 August 2006
- journal article
- Published by American Diabetes Association in Diabetes Care
- Vol. 29 (8) , 1909-1914
- https://doi.org/10.2337/dc06-0438
Abstract
OBJECTIVE—To compare the pathophysiology of impaired fasting glucose (IFG) and impaired glucose tolerance (IGT) in a more comprehensive and standardized fashion than has hitherto been done. RESEARCH DESIGN AND METHODS—We studied 21 individuals with isolated IFG (IFG/normal glucose tolerance [NGT]), 61 individuals with isolated IGT (normal fasting glucose [NFG]/IGT), and 240 healthy control subjects (NFG/NGT) by hyperglycemic clamps to determine first- and second-phase insulin release and insulin sensitivity. Homeostasis model assessment (HOMA) indexes of β-cell function (HOMA-%B) and insulin resistance (HOMA-IR) were calculated from fasting plasma insulin and glucose concentrations. RESULTS—Compared with NFG/NGT, IFG/NGT had similar fasting insulin concentrations despite hyperglycemia; therefore, HOMA-IR was increased ∼30% (P < 0.05), but clamp-determined insulin sensitivity was normal (P > 0.8). HOMA-%B and first-phase insulin responses were reduced ∼35% (P < 0.002) and ∼30% (P < 0.02), respectively, but second-phase insulin responses were normal (P > 0.5). NFG/IGT had normal HOMA-IR but ∼15% decreased clamp-determined insulin sensitivity (P < 0.03). Furthermore, HOMA-%B was normal but both first-phase (P < 0.0003) and second-phase (P < 0.0001) insulin responses were reduced ∼30%. IFG/NGT differed from NFG/IGT by having ∼40% lower HOMA-%B (P < 0.012) and ∼50% greater second-phase insulin responses (P < 0.005). CONCLUSIONS—Since first-phase insulin responses were similarly reduced in IFG/NGT and NFG/IGT, we conclude that IFG is due to impaired basal insulin secretion and preferential resistance of glucose production to suppression by insulin, as reflected by fasting hyperglycemia despite normal plasma insulin concentrations and increased HOMA-IR, whereas IGT mainly results from reduced second-phase insulin release and peripheral insulin resistance, as reflected by reduced clamp-determined insulin sensitivity.Keywords
This publication has 24 references indexed in Scilit:
- Follow-up Report on the Diagnosis of Diabetes MellitusDiabetes Care, 2003
- Insulin secretion and action show differences in impaired fasting glucose and in impaired glucose tolerance in Asian IndiansDiabetes/Metabolism Research and Reviews, 2003
- Relative contributions of β-cell function and tissue insulin sensitivity to fasting and postglucose-load glycemiaMetabolism, 2000
- Impaired glucose tolerance and fasting hyperglycaemia have different characteristicsDiabetic Medicine, 2000
- Pancreatic beta-cell dysfunction as the primary genetic lesion in NIDDM. Evidence from studies in normal glucose-tolerant individuals with a first-degree NIDDM relativePublished by American Medical Association (AMA) ,1995
- Quantification of the relationship between insulin sensitivity and beta-cell function in human subjects. Evidence for a hyperbolic functionDiabetes, 1993
- Carbohydrate Metabolism in Non-Insulin-Dependent Diabetes MellitusNew England Journal of Medicine, 1992
- Role of Reduced Suppression of Glucose Production and Diminished Early Insulin Release in Impaired Glucose ToleranceNew England Journal of Medicine, 1992
- Die euglykämische Insulin- und hyperglykämische Clamp-TechnikTransfusion Medicine and Hemotherapy, 1984
- Use of a heated superficial hand vein as an alternative site for the measurement of amino acid concentrations and for the study of glucose and alanine kinetics in manMetabolism, 1981