Abstract

The long-term objective of this laboratory is to understand the mechanism of insulin resistance in the human liver from patients with NIDDM. This new effort is possible because: 1) a method to isolate and culture insulin-responsive hepatocytes from an open liver biopsy has been developed, and 2) ECU School of Medicine has a population of patients from whom an intraoperative liver biopsy can be obtained. Over 100 gastric bypass procedures are performed annually for the treatment of morbid obesity, of whom 27% have NIDDM, 20% impaired glucose tolerance, and the rest have normal glucose tolerance. Initial studies with isolated hepatocytes from these and other non- obese, non-diabetic patients undergoing elective surgery will establish the interrelationships between insulin action, binding, internalization, and degradation. Then, insulin receptor structure, metabolism and function, and the level and abundance of the various species of the insulin receptor mRNA will be studied before the intracellular domain can be assigned as the site for the defect in NIDDM. We will test the hypothesis that in NIDDM hyperglycemia causes nonenzymatic glycosylation of the insulin receptor and alters its function. Also, in addition to determining the activity of the insulin receptor kinase in vitro and in vivo, strategies are developed to demonstrate phosphorylation of endogenous substrates by the insulin receptor kinase. Finally, analytical and enzymatic methods will be used in isolated hepatocytes and liver homogenates to ascertain if the carbohydrate intolerance of NIDDM is due to increased glucose production, decreased glucose utilization, or a combination of both. Special effort will be given to two important regulatory loci: 1) pyruvate dehydrogenase activity, the critical link enzyme between carbohydrate and lipid metabolism, and 2) fructose 2,6- bisphosphate concentration, a key compound in the control of glucose metabolism. The significance of this proposal is enhanced by the recognition that the background knowledge from human liver at the cellular level is virtually nonexistent. It is hoped that this work will establish the cellular basis for the insulin resistance in NIDDM and help to develop a more rational therapeutic approach to the disease.

  Funding Agency

Agency
National Institute of Health (NIH)
Institute
National Institute of Diabetes and Digestive and Kidney Diseases (NIDDK)
Type
Research Program Projects (P01)
Project #
5P01DK036296-02
Application #
3917986
Study Section
Project Start
Project End
Budget Start
Budget End
Support Year
2
Fiscal Year
1988
Total Cost
Indirect Cost

  Institution

Name
East Carolina University
Department
Type
DUNS #
City
Greenville
State
NC
Country
United States
Zip Code
27858

  Publications

Friedman, J E; Caro, J F; Pories, W J et al. (1994) Glucose metabolism in incubated human muscle: effect of obesity and non-insulin-dependent diabetes mellitus. Metabolism 43:1047-54
Long, S D; O'Brien, K; MacDonald Jr, K G et al. (1994) Weight loss in severely obese subjects prevents the progression of impaired glucose tolerance to type II diabetes. A longitudinal interventional study. Diabetes Care 17:372-5
Elton, C W; Tapscott, E B; Pories, W J et al. (1994) Effect of moderate obesity on glucose transport in human muscle. Horm Metab Res 26:181-3
Houmard, J A; Shinebarger, M H; Dolan, P L et al. (1993) Exercise training increases GLUT-4 protein concentration in previously sedentary middle-aged men. Am J Physiol 264:E896-901
Houmard, J A; Hortobagyi, T; Neufer, P D et al. (1993) Training cessation does not alter GLUT-4 protein levels in human skeletal muscle. J Appl Physiol 74:776-81
Friedman, J E; Dohm, G L; Leggett-Frazier, N et al. (1992) Restoration of insulin responsiveness in skeletal muscle of morbidly obese patients after weight loss. Effect on muscle glucose transport and glucose transporter GLUT4. J Clin Invest 89:701-5
Caro, J F; Jenquin, M; Long, S (1992) Effects of phorbol esters on insulin receptor function and insulin action in hepatocytes: evidence for heterogeneity. Mol Cell Biochem 109:115-8
Contreras, I; Caro, J F; Aveledo, L et al. (1992) In chronic uremia, insulin activates receptor kinase but not pyruvate dehydrogenase. Nephron 61:77-81
Pories, W J; MacDonald Jr, K G; Flickinger, E G et al. (1992) Is type II diabetes mellitus (NIDDM) a surgical disease? Ann Surg 215:633-42;discussion 643
Barakat, H A; McLendon, V D; Marks, R et al. (1992) Influence of morbid obesity and non-insulin-dependent diabetes mellitus on high-density lipoprotein composition and subpopulation distribution. Metabolism 41:37-41

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