Genetic Susceptibility to Adverse Metabolic Consequences of Obesity
Project Number1RL1HL092550-01
Contact PI/Project LeaderCOHEN, JONATHAN C
Awardee OrganizationUT SOUTHWESTERN MEDICAL CENTER
Description
Abstract Text
The prevalence of obesity is burgeoning in the United States. As a result, obesity-related metabolic disorders
that confer increased CVD risk, including diabetes, dyslipidemia, and hypertension are reaching epidemic
proportions. Susceptibility to the adverse metabolic consequences of obesity varies widely in the population:
modest increases in adiposity lead to severe metabolic decompensation in some individuals, whereas others
maintain a normal metabolic profile despite severe obesity. The overall goal of this project is to identify
specific genetic mechanisms that account for the variability of metabolic responses to excess body weight
and to evaluate the therapeutic potential of agents that target these mechanisms. The study includes three
complementary strategies: First, we will sequence selected candidate genes in a large, multi-ethnic
population (The Dallas Heart Study) in which each participant has undergone extensive metabolic
characterization and relate the phenotypes to selected genotypes. Our focus will be on two groups of genes:
1) genes encoding circulating proteins that carry metabolic signals between the brain, liver, adipose tissue,
and intestine ('metabokines'), and 2) genes encoding selected transcriptional regulatory molecules than
respond to metabolic signals ('cellular metabolic regulators'). Included in these studies are genes being
mechanistically interrogated in Projects 1-3. Second, we will use genome-wide methods as unbiased
approaches toward the discovery of new genes and sequence variants that contribute to inter-individual
differences in the metabolic responses to obesity. Third, we will collaborate with investigators in Projects 4
& 5 and perform detailed studies of glucose and lipid metabolism in both mice and humans to elucidate the
mechanistic basis for genetic variation in susceptibility to the adverse metabolic consequences of obesity.
This ambitious, interdisciplinary program leverages our established strengths in pairing careful phenotypic
characterization with comprehensive genetic analyses in humans to discover new genes and sequence
variations contributing to metabolic traits. In addition we have established collaborations that provide access
to large, prospective population studies in which the effects of genetic sequence variants can be rigorously
validated. These collaborations, together with the complementary expertise of our collaborators in Projects
1-5 greatly expand the scientific scope of our studies and increases our potential to identify new therapeutic
targets and approaches to prevent and treat the adverse metabolic consequences of obesity.
No Sub Projects information available for 1RL1HL092550-01
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