Abstract

Five naturally occurring mutations causing obesity have been mapped in the mouse: agouti, obese, diabetes, tub, and fat. This represents an important contribution to understanding the pathophysiology of obesity. The diverse nature of the gene products associated with the obese phenotype suggests that the pathophysiology of obesity is indeed heterogeneous. At the same time, the observation that identical mutations exert different effects in different mouse strains suggest that a panoply of genes interacts with the susceptibility allele. Identification of such interacting or modifier genes is the goal of the present proposal. Because of the heterogeneous and polygenic nature of human obesity, it is not surprising that defects in single genes such as leptin or CPE do not appear to be associated with common forms of obesity in man. The rationale of the present proposal is that the modifier genes may play a more important role in the pathophysiology of common forms of obesity. The fat mutation arose spontaneously in the inbred HRS/J (HRS) strain. The fat mutation had been shown to be associated with hyperinsulinemia. In previous work, the PI showed that hyperinsulinemia in fat mice is primarily due to hyperproinsulinemia, which precedes obesity and is independent of hyperglycemia. CPE is the enzyme required for processing the proinsulin molecule by removing the carboxy-terminal diarginyl residue. In addition, CPE catalyzes processing of other peptide hormones, such as POMC, neurotensin and CCK. A point mutation in the CPE gene causing a single missense mutation in the CPE molecule has been identified as the fat mutation. The correlation between the mutant allele of CPE and the development of obesity is unclear. Interestingly, humans with familial forms of hyperproinsulinemia do not develop obesity, but a single case of a defect in the prohormone convertase gene (PC 1) has been associated with development of massive obesity in man. It is possible that the processing defect affects multiple hormones, thereby causing multiple metabolic defects. Interestingly, the genetic background of the fat mutation affects the phenotype, so that on the HRS background, the fat mutation gives rise to obesity without hyperglycemia, whereas on the C57BLKS/J background (BKS), the fat mutation gives rise to obesity and hyperglycemia.

  Funding Agency

Agency
National Institute of Health (NIH)
Institute
National Institute of Diabetes and Digestive and Kidney Diseases (NIDDK)
Type
Research Project (R01)
Project #
1R01DK053278-01
Application #
2448049
Study Section
Metabolism Study Section (MET)
Program Officer
Laughlin, Maren R
Project Start
1998-03-18
Project End
2003-01-31
Budget Start
1998-03-18
Budget End
1999-01-31
Support Year
1
Fiscal Year
1998
Total Cost
Indirect Cost

  Institution

Name
Jackson Laboratory
Department
Type
DUNS #
042140483
City
Bar Harbor
State
ME
Country
United States
Zip Code
04609

  Publications

Collin, Gayle B; Maddatu, Terry P; Sen, Saunak et al. (2005) Genetic modifiers interact with Cpe(fat) to affect body weight, adiposity, and hyperglycemia. Physiol Genomics 22:182-90
Collin, G B; Marshall, J D; Boerkoel, C F et al. (1999) Alstrom syndrome: further evidence for linkage to human chromosome 2p13. Hum Genet 105:474-9
Kim, J H; Nishina, P M; Naggert, J K (1998) Genetic models for non insulin dependent diabetes mellitus in rodents. J Basic Clin Physiol Pharmacol 9:325-45