Abstract

? ? More than 26 percent of the U.S. population has a body mass index (BMI) in excess of 30 and thus qualifies as obese. Although heritability is a well-established factor in the development of obesity, the genes underlying this tendency have been difficult to identify. One of the few monogenic forms of obesity identified to date results from mutations GPCR, MC4R. In light of this precedent and the need to define more common explanations underlying genetic susceptibility to obesity, it is of particular note that pharmacologic and/or genetic evidence has implicated more than twenty GPCRs as modulators of food intake, body weight and/or the hedonic (i.e., rewarding) response to feeding. The vast majority of these receptors have multiple known non-synonymous (i.e., changes in coding sequence) variants. By analyzing the prevalence, pharmacologic function, and co-existence of GPCR polymorphisms in the Look AHEAD population we will test our central hypothesis that a significant portion of obesity in the general population is linked with abnormal GPCR function. We will first define the MC4R variants (known and novel) in the Look AHEAD population by sequence and haplotype analysis.
Aim 1 will provide insight into the role of this receptor in a large cohort of obese diabetic subjects as well as address the controversy surrounding the extent to which a known common variant (VI031) is protective against obesity. In addition, study of the MC4R will establish a baseline on which to explore the importance of other factors (e.g., GPCR polymorphisms) as genetic determinants of body weight. Furthermore, the analysis of the MC4R will enable other Look AHEAD investigators to take this variable into account as a potentially confounding factor in defining clinical susceptibilities.
In Aim 2, we will genotype non-synonymous coding region polymorphisms and haplotype markers in a series of twenty orexigenic, anorexigenic and hedonic GPCRs postulated to have an etiologic role in the development of obesity. These receptor variants have been identified from the NCBI SNP database and from the literature. In parallel, corresponding mutant recombinant GPCRs will be expressed in heterologous cell lines and pharmacologically assessed. Polymorphic receptors will be classified as gain of function, loss of function, or wild type. The correlation between functional abnormalities and phenotypic parameters will be assessed within the study population.
In Aim 3, combinations of anorexigenic, orexigenic and hedonic receptor variants will be assessed as potential synergistic or additive factors underlying the polygenic basis of obesity and/or other Look AHEAD study endpoints. ? ?

  Funding Agency

Agency
National Institute of Health (NIH)
Institute
National Institute of Diabetes and Digestive and Kidney Diseases (NIDDK)
Type
Research Project (R01)
Project #
5R01DK072497-03
Application #
7249490
Study Section
Special Emphasis Panel (ZDK1-GRB-N (M2))
Program Officer
Karp, Robert W
Project Start
2005-09-15
Project End
2010-06-30
Budget Start
2007-07-01
Budget End
2008-06-30
Support Year
3
Fiscal Year
2007
Total Cost
$758,848
Indirect Cost

  Institution

Name
Tufts University
Department
Type
DUNS #
079532263
City
Boston
State
MA
Country
United States
Zip Code
02111

  Publications

Doyle, Jamie R; Krishnaji, Subrahmanian T; Zhu, Guangli et al. (2014) Development of a membrane-anchored chemerin receptor agonist as a novel modulator of allergic airway inflammation and neuropathic pain. J Biol Chem 289:13385-96
Doyle, Jamie R; Lane, Jacqueline M; Beinborn, Martin et al. (2013) Naturally occurring HCA1 missense mutations result in loss of function: potential impact on lipid deposition. J Lipid Res 54:823-30
McCaffery, J M; Papandonatos, G D; Huggins, G S et al. (2013) FTO predicts weight regain in the Look AHEAD clinical trial. Int J Obes (Lond) 37:1545-52
Doyle, J R; Fortin, J P; Beinborn, M et al. (2012) Selected melanocortin 1 receptor single-nucleotide polymorphisms differentially alter multiple signaling pathways. J Pharmacol Exp Ther 342:318-26
McCaffery, Jeanne M; Papandonatos, George D; Peter, Inga et al. (2012) Obesity susceptibility loci and dietary intake in the Look AHEAD Trial. Am J Clin Nutr 95:1477-86
Peter, Inga; McCaffery, Jeanne M; Kelley-Hedgepeth, Alyson et al. (2012) Association of type 2 diabetes susceptibility loci with one-year weight loss in the look AHEAD clinical trial. Obesity (Silver Spring) 20:1675-82
Fortin, Jean-Philippe; Chinnapen, Daniel; Beinborn, Martin et al. (2011) Discovery of dual-action membrane-anchored modulators of incretin receptors. PLoS One 6:e24693
Smart-Halajko, Melissa C; Kelley-Hedgepeth, Alyson; Montefusco, Maria Claudia et al. (2011) ANGPTL4 variants E40K and T266M are associated with lower fasting triglyceride levels in Non-Hispanic White Americans from the Look AHEAD Clinical Trial. BMC Med Genet 12:89
Pugliese-Pires, Patricia N; Fortin, Jean-Philippe; Arthur, Thais et al. (2011) Novel inactivating mutations in the GH secretagogue receptor gene in patients with constitutional delay of growth and puberty. Eur J Endocrinol 165:233-41
Fortin, Jean-Philippe; Ci, Lei; Schroeder, Jonathan et al. (2010) The ýý-opioid receptor variant N190K is unresponsive to peptide agonists yet can be rescued by small-molecule drugs. Mol Pharmacol 78:837-45

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