Abstract

Obesity develops when energy intake exceeds energy expenditure, leading to an accumulation of adipose tissue. The pandemic of excess adipose tissue is of increasing importance throughout the world. In addition to its own specific morbidities, obesity is linked to insulin resistance and the devastating metabolic syndrome of type 2 diabetes. The intricate balance of energy homeostasis is tightly regulated by a complex network of metabolic genes which respond to changing environmental conditions. Transcriptional regulation has recently been shown to extensively modulate adipocyte biology. We have discovered that a novel transcriptional coregulator, TRIP-Br2, is critical for maintaining energy homeostasis in mice. Our preliminary data from preadipocyte cell lines and TRIP-Br2 null mice leads us to propose an important role of TRIP-Br2 in adipocyte biology. Thus, the goal of this proposal is to determine the function and mechanism of TRIP-Br2 in energy metabolism in adipose tissue. I will test the hypothesis that disruption of TRIP-Br2 protects mice from diet- induced obesity through upregulation of energy expenditure with three specific aims.
For Specific Aim 1, I will physically and physiologically examine the TRIP-Br2 null mice to identify the in vivo mechanism for diet- induced obesity resistance observed in TRIP-Br2 KO mice. Completion of Aim 1, which will take place during K99 phase, will provide me with training in aspects of in vivo and ex vivo adipose physiology necessary to independently complete the R00 phase.
For Specific Aim 2, which will span the K99 and R00 phases, I will determine the molecular targets of TRIP-Br2 that contribute to the diet-induced obesity resistance phenotype in TRIP-Br2 null mice using genome-wide gene and protein expressions together with bioinformatics analysis. Completion of the subaim of Aim 2 proposed during the K99 phase will provide me with the training in analysis of complex datasets with computational biology necessary to independently to complete Aim 2 during the R00 phase.
For Specific Aim 3 (R00 phase), I will determine the composition of TRIP-Br2 transcriptional regulatory complex in adipocytes. Completion of this aim will allow me to link the TRIP-Br2 regulatory network with known gene regulatory system in adipocyte. These experiments are novel in that they combine mouse genetic, physiologic, and molecular biology approaches to examine the mechanistic role of TRIP-Br2 in energy metabolism. These studies will provide novel insights into the transcriptional regulation of adipocyte function and could potentially be used for developing therapeutic targets for obesity.

Public Health Relevance

Obesity is a critical health problem in the US because it leads to fatal complications. These studies will determine the mechanisms contributing to high fat diet-induced obesity resistance in our mouse model. Understanding the gene targets will facilitate development of therapeutic strategies.

  Funding Agency

Agency
National Institute of Health (NIH)
Institute
National Institute of Diabetes and Digestive and Kidney Diseases (NIDDK)
Type
Career Transition Award (K99)
Project #
1K99DK090210-01
Application #
8028935
Study Section
Diabetes, Endocrinology and Metabolic Diseases B Subcommittee (DDK)
Program Officer
Haft, Carol R
Project Start
2010-09-25
Project End
2012-08-31
Budget Start
2010-09-25
Budget End
2011-08-31
Support Year
1
Fiscal Year
2010
Total Cost
$90,000
Indirect Cost

  Institution

Name
Joslin Diabetes Center
Department
Type
DUNS #
071723084
City
Boston
State
MA
Country
United States
Zip Code
02215

  Publications

Qi, Weier; Li, Qian; Liew, Chong Wee et al. (2017) SHP-1 activation inhibits vascular smooth muscle cell proliferation and intimal hyperplasia in a rodent model of insulin resistance and diabetes. Diabetologia 60:585-596
Kawamori, Dan; Shirakawa, Jun; Liew, Chong Wee et al. (2017) GLP-1 signalling compensates for impaired insulin signalling in regulating beta cell proliferation in ?IRKO mice. Diabetologia 60:1442-1453
Molven, Anders; Hollister-Lock, Jennifer; Hu, Jiang et al. (2016) The Hypoglycemic Phenotype Is Islet Cell-Autonomous in Short-Chain Hydroxyacyl-CoA Dehydrogenase-Deficient Mice. Diabetes 65:1672-8
Qiang, Guifen; Kong, Hyerim Whang; Fang, Difeng et al. (2016) The obesity-induced transcriptional regulator TRIP-Br2 mediates visceral fat endoplasmic reticulum stress-induced inflammation. Nat Commun 7:11378
El Ouaamari, Abdelfattah; Dirice, Ercument; Gedeon, Nicholas et al. (2016) SerpinB1 Promotes Pancreatic ? Cell Proliferation. Cell Metab 23:194-205
Bhatt, Shweta; Gupta, Manoj K; Khamaisi, Mogher et al. (2015) Preserved DNA Damage Checkpoint Pathway Protects against Complications in Long-Standing Type 1 Diabetes. Cell Metab 22:239-52
El Ouaamari, Abdelfattah; Zhou, Jian-Ying; Liew, Chong Wee et al. (2015) Compensatory Islet Response to Insulin Resistance Revealed by Quantitative Proteomics. J Proteome Res 14:3111-3122
Liew, Chong Wee; Assmann, Anke; Templin, Andrew T et al. (2014) Insulin regulates carboxypeptidase E by modulating translation initiation scaffolding protein eIF4G1 in pancreatic ? cells. Proc Natl Acad Sci U S A 111:E2319-28
Akiyama, Masaru; Liew, Chong Wee; Lu, Shusheng et al. (2013) X-box binding protein 1 is essential for insulin regulation of pancreatic ?-cell function. Diabetes 62:2439-49
Liew, Chong Wee; Boucher, Jeremie; Cheong, Jit Kong et al. (2013) Ablation of TRIP-Br2, a regulator of fat lipolysis, thermogenesis and oxidative metabolism, prevents diet-induced obesity and insulin resistance. Nat Med 19:217-26

Showing the most recent 10 out of 13 publications