| Literature DB >> 31910156 |
Yang Chen1, Mingyue Zhao2, Chenhao Wang3, Huaizhen Wen4, Yuntao Zhang5, Mingxu Lu6, Salah Adlat7, Tingting Zheng8, Mingjiao Zhang9, Dan Li10, Xiaodan Lu11, Mengwei Guo12, Hongyu Chen13, Luqing Zhang14, Xuechao Feng15, Yaowu Zheng16.
Abstract
Excessive fat accumulation causes obesity and many diseases. Previous study demonstrates VEGFB universal knockout induces obese phenotypes including expansion of white adipose tissue, whitening of brown adipose tissue, increase of fat accumulation and reduction in energy consumption. However, roles of VEGFB in adipose tissues are not clear. In this study, we have generated a mouse model with adipose-specific VEGFB repression using CRISPR/dCas9 system (VegfbAdipoDown) and investigated the roles of VEGFB in adipose development and energy metabolism. VEGFB repression induced significant changes in adipose tissue structure and function. VegfbAdipoDown mice have larger body sizes, larger volume of white adipose tissues than its wild type littermates. Adipose-specific VEGFB repression induced morphological and functional transformation of adipose tissues toward white adipose for energy storage. Metabolic processes are broadly changed in VegfbAdipoDown adipose tissues including carbohydrate metabolism, lipid metabolism, nucleotide metabolism and amino acid metabolism. We have demonstrated that adipose VEGFB repression can recapitulate most of the phenotypes of the whole body VEGFB knockout mouse. Intriguingly, approximately 50% VEGFB repression in adipose tissues can almost completely mimic the effects of universal Vegfb deletion, suggesting adipose VEGFB is a major regulator of energy metabolism and may be important in prevention and treatment of obesity.Entities:
Year: 2020 PMID: 31910156 DOI: 10.1530/JOE-19-0341
Source DB: PubMed Journal: J Endocrinol ISSN: 0022-0795 Impact factor: 4.286