Fibroblast Growth Factor and Energy Metabolism

成纤维细胞生长因子和能量代谢

• 批准号: 10597660
• 负责人: Yu-Hua Tseng
• 金额: $ 54.87万
• 依托单位: JOSLIN DIABETES CENTER
• 依托单位国家: 美国
• 财政年份: 2015
• 资助国家: 美国
• 起止时间: 2015-07-03 至 2025-03-31
• 项目状态: 未结题
• 来源: https://reporter.nih.gov/project-details/10597660
• 关键词: Adipocytes; Adipose tissue; Automobile Driving; Blood Vessels; Brown Fat; Calories; Cell Differentiation process; Cell Fraction; Cell Proliferation; Cell Separation; Chromatin; Chromatin Remodeling Factor; Complex; DNA Methylation; Data; Diabetes Mellitus; Disease; Dissociation; Endocrine; Endothelial Cells; Endothelium; Energy Metabolism; Epidemic; Epigenetic Process; FGF9 gene; FGFR3 gene; Fatty acid glycerol esters; Fibroblast Growth Factor; Gene Expression; Genes; Genetic Transcription; Goals; Grant; Growth Factor; Health; In Vitro; Knockout Mice; Knowledge; Ligands; Lipids; Mammals; Maps; Mediating; Metabolic Diseases; Metabolic syndrome; Mitochondria; Modeling; Mus; Nanotechnology; Non-Insulin-Dependent Diabetes Mellitus; Nuclear Receptors; Obesity; Pathology; Pathway interactions; Physiological; Play; Protein Engineering; Proteins; Regulation; Research; Rodent; Role; Scheme; Signal Transduction; Stimulus; System; Therapeutic; Thermogenesis; United States; Vascular Endothelial Cell; Vascularization; adipokines; angiogenesis; autocrine; combat; comorbidity; delivery vehicle; epigenetic regulation; fibroblast growth factor 6; fibroblast growth factor 9; gain of function; glucose tolerance; histone modification; improved; in vivo; innovation; insulin sensitivity; intercellular communication; lipid biosynthesis; loss of function; mouse model; nanoparticle; neovascularization; novel; novel therapeutics; obesity prevention; precursor cell; progenitor; programs; receptor; recruit; response; single-cell RNA sequencing; stem cells; success; uncoupling protein 1

Project Summary/Abstract Obesity is growing at epidemic rates worldwide and leads to a broad spectrum of other disorders, which collectively form metabolic syndrome. Central to these pathologies is the adipose tissue. In mammals, there are two functionally distinct types of fat: white adipose tissue, which stores excess calories, and brown and its related beige adipose tissue, which dissipates energy for thermogenesis. Numerous studies in rodents have demonstrated that increasing the amount or activity of brown or beige fat holds excellent therapeutic potential for obesity-related metabolic diseases. Adipose tissue undergoes dramatic remodeling in response to environmental challenges. Cold exposure is an effective way to increase brown fat mass and activity. as well as to induce browning of white adipose tissue. While it has long been postulated that growth factors produced by the adipose niche play a critical role in the remodeling of brown and white fat upon cold challenge, the identity of such factors have remained mostly unidentified. Recently, we discovered that fibroblast growth factor (FGF) 9 is a cold-induced adipokine and can induce UCP1 expression independent of brown adipogenesis. In addition to adipose progenitors, FGF9 also stimulates thermogenic program in mature adipocytes. Importantly, expression of FGF receptor 3 (FGFR3), the receptor that mediates FGF9’s effects, is also induced by cold in both the stromal vascular fraction (SVF) cells and adipocytes, suggesting that FGF9 functions as an autocrine/endocrine factor within the adipose niche. Using single-cell RNA sequencing of the adipose SVF, we identify FGFR3’s abundant expression in the vascular endothelial cells. Based on these exciting findings, we hypothesize that FGF9, produced by adipocytes, functions as a niche factor to promote brown and white adipose tissue remodeling and modulate thermogenic program in mature adipocytes, in response to cold challenge. The primary goals of this grant are to 1) determine the role of FGF9 in regulation of thermogenic program in mature adipocytes and delineate the underlying transcriptional and epigenetic mechani, 2) determine the role of FGF9-induced angiogenesis in adipose remodeling, and 3) use both gain- and loss-of-function mouse models and nanotechnology to define the in vivo role of the FGF9-FGFR3 axis in energy metabolism and explore the potential of targeting this pathway to develop new therapies to treat obesity and its many related co-morbidities. Completion of the proposed studies will lead to a new understanding of adipose remodeling and could provide potential therapeutic approaches for obesity, type 2 diabetes, and other related metabolic diseases.

项目总结/文摘