Insulin Sensitivity and Acute Insulin Response in African-Americans, Non-Hispanic Whites, and Hispanics With NIDDM: The Insulin Resistance Atherosclerosis Study

Author:

Haffner Steven M1,Howard George2,Mayer Elizabeth2,Bergman Richard N3,Savage Peter J4,Rewers Marian5,Mykkänen Leena6,Karter Andrew J7,Hamman Richard5,Saad Mohammed F8

Affiliation:

1. Department of Medicine, University of Texas Health Science Center San Antonio, Texas

2. Bowman Gray School of Medicine, Department of Public Health Sciences Winston-Salem, North Carolina

3. University of Southern California School of Medicine, Department of Physiology and Biophysics Los Angeles, California

4. National Institutes of Health, National Heart, Lung and Blood Institute, Division of Epidemiology and Clinical Applications Bethesda, Maryland

5. University of Colorado School of Medicine, Department of Preventive Medicine and Biometrics Denver, Colorado

6. Department of Medicine, University of Kuopio Kuopio, Finland

7. Kaiser Permanente, Division of Research Oakland, California

8. University of Southern California, School of Medicine, Department of Medicine Los Angeles, California

Abstract

NIDDM is usually characterized by β-cell failure decreased and insulin sensitivity. It has been reported that a high proportion of African-American NIDDM subjects are insulin sensitive. To examine this issue, we determined insulin sensitivity (SI) in 479 NIDDM subjects by minimal model analyses of frequently sampled intravenous glucose tolerance (FSIGT) from the Insulin Resistance Atherosclerosis Study (IRAS), a large multicenter study of insulin sensitivity and cardiovascular risk in African-Americans, Hispanics, and non-Hispanic whites. The African-Americans and non-Hispanic whites were sampled in Los Angeles and Oakland, California. The non-Hispanic whites and Hispanics were sampled in San Antonio, Texas, and San Luis Valley, Colorado. We defined the proportion of insulin-sensitive (SI) subjects as ≥1.61 min−1 · μU−1 · ml−1, which is above the median for nondiabetic subjects of all ethnic groups in the IRAS. Using this definition, the proportion of insulin-sensitive diabetic subjects was very low in all ethnic groups (non-Hispanic whites [14.3%] vs. African- Americans [6.5%], P = 0.039 in Los Angeles and Oakland; non-Hispanic whites [6.8%] vs. Hispanics [4.9%], P = 0.737 in San Luis Valley and San Antonio). These results were also similar in newly diagnosed mildly hyperglycemic diabetic subjects. In addition, these results were not affected by the adjustment for differences in obesity, body fat distribution, and severity of hyperglycemia. Even in nonobese subjects (with BMI <30 kg/m2), the proportion of insulin-sensitive subjects (S1 ≥1.61 min−1 · μU−1 · ml−1) was low (3.6–9.7%). The acute insulin response (AIR) was significantly higher in African-Americans than in non-Hispanic whites; there were no ethnic differences in AIR between Hispanics and non–Hispanic whites. There were no significant ethnic differences for non-insulin-mediated glucose disposal (SG). We conclude that the number of insulinsensitive NIDDM subjects is low and similar among non-Hispanic whites, Hispanics, and African-Americans in the U.S.

Publisher

American Diabetes Association

Subject

Endocrinology, Diabetes and Metabolism,Internal Medicine

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