Abstract

Obesity is a major health problem spreading at an epidemic pace throughout the world without any sign of abatement. Development of obesity, which is often associated with insulin resistance and diabetes, results from an excess of energy intake over expenditure. Brown adipose tissues (BAT) have the unique ability to burn excess calories, and facilitate triglyceride clearance and glucose disposal. Previously, we identified Follistatin (Fst) as a direct target of testosterone that regulates skeletal muscle mass and inhibits transforming growth factor- (TGF-) signaling. Based on our preliminary findings, we hypothesize that Fst promotes overall thermogenic program and improves symptoms of obesity and metabolic disorder by regulating overall Mst/TGF-/BMP/Myf5/PRDM16- signaling pathways. We will test our hypothesis with the following Specific Aims- Aim 1: We will demonstrate the essential role of Fst during brown fat differentiation and the regulation of thermogenic program in vitro and in vivo.
Aim 2 : We will determine the molecular mechanisms by which Fst regulates the overall thermogenic program and Aim 3: We will generate mice expressing Fst under the control of adiponectin or UCP1 regulatory elements, and compare their metabolic parameters and response to high fat chow diet with control littermates. We will determine the effect of endogenous and exogenous Fst on protein and gene expression profiles of key thermogenic markers, and overall cellular bioenergetics using both in vitro and in vivo models under basal and -adrenoceptor agonist (CL316,248) stimulated conditions. Involvement of Myf5/PRDM16, Mst/pSmad2/3/BMP/COX 2, insulin receptor and AMPK/PGC-1? signaling pathway in in vitro models as well as in adiponectin-Fst and UCP1-Fst transgenic mice will be analyzed by Affymetrix gene expression and quantitative western blot analysis. Expression levels of Fst, Myf5 and Smad3 in mouse preadipocytes and MEF cultures will be inhibited by siRNAs and their thermogenic capabilities will be determined. We will generate Fst-transgenic mice using adiponectin (Adipoq) and UCP1-specific promoters, and test the effect of high fat diet on their body composition (Micro CT), energy expenditure (indirect calorimetric analysis), insulin sensitivity and glucose tolerance under both basal and ?-adrenoceptor agonist (CL 316,248) stimulated conditions. Serum levels of Fst, adiponectin and lipid profiles will be analyzed by ELISA. Evaluating the critical role of Fst during its regulation of overall thermogenic process will provide rationale for novel therapeutic drug design for the treatment of obesity and related metabolic diseases.

Public Health Relevance

This project will test the role of follistatin (Fst) in regulating overall thermogenic program in in vitro and in vivo models. Mouse brown preadipocyte and embryonic fibroblast cultures obtained from WT and Fst null (Fst KO) embryos will be analyzed for the expression of thermogenic markers either in presence or absence of Fst. We will also analyze the molecular mechanisms that may be responsible for the pro-thermogenic action of Fst. We will generate transgenic mice that will over-express Fst specifically in white or brown adipose tissues and study their thermogenic capability as well as their response to high fat diet on their body composition and metabolic parameters. Our studies if validated by our preliminary data will provide unique approach to regulate thermogenic programming and treatment of obesity and related metabolic diseases.

  Funding Agency

Agency
National Institute of Health (NIH)
Institute
National Institute on Aging (NIA)
Type
Research Enhancement Award (SC1)
Project #
5SC1AG049682-06
Application #
8900887
Study Section
Special Emphasis Panel (ZGM1-TWD-6 (SC))
Program Officer
Kohanski, Ronald A
Project Start
2014-08-01
Project End
2018-05-31
Budget Start
2015-06-15
Budget End
2016-05-31
Support Year
6
Fiscal Year
2015
Total Cost
$287,000
Indirect Cost
$87,000

  Institution

Name
Charles R. Drew University of Medicine & Science
Department
Internal Medicine/Medicine
Type
Schools of Medicine
DUNS #
785877408
City
Los Angeles
State
CA
Country
United States
Zip Code
90059

  Publications

Singh, Rajan; Pervin, Shehla; Lee, Se-Jin et al. (2018) Metabolic profiling of follistatin overexpression: a novel therapeutic strategy for metabolic diseases. Diabetes Metab Syndr Obes 11:65-84
Pervin, Shehla; Singh, Vineeta; Tucker, Alexandria et al. (2017) Modulation of transforming growth factor-?/follistatin signaling and white adipose browning: therapeutic implications for obesity related disorders. Horm Mol Biol Clin Investig 31:
Singh, Rajan; Braga, Melissa; Reddy, Srinivasa T et al. (2017) Follistatin Targets Distinct Pathways To Promote Brown Adipocyte Characteristics in Brown and White Adipose Tissues. Endocrinology 158:1217-1230
Martinez, Luis; Thames, Easter; Kim, Jinna et al. (2016) Increased sensitivity of African American triple negative breast cancer cells to nitric oxide-induced mitochondria-mediated apoptosis. BMC Cancer 16:559
Singh, Rajan; Parveen, Meher; Basgen, John M et al. (2016) Increased Expression of Beige/Brown Adipose Markers from Host and Breast Cancer Cells Influence Xenograft Formation in Mice. Mol Cancer Res 14:78-92
Singh, Rajan; Braga, Melissa; Pervin, Shehla (2014) Regulation of brown adipocyte metabolism by myostatin/follistatin signaling. Front Cell Dev Biol 2:60
Braga, Melissa; Reddy, Srinivasa T; Vergnes, Laurent et al. (2014) Follistatin promotes adipocyte differentiation, browning, and energy metabolism. J Lipid Res 55:375-84