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SOX4 facilitates brown fat development and maintenance through EBF2-mediated thermogenic gene program in mice

Cell death and differentiation. 2024-10; 
Shuai Wang, Ting He, Ya Luo, Kexin Ren, Huanming Shen, Lingfeng Hou, Yixin Wei, Tong Fu, Wenlong Xie, Peng Wang, Jie Hu, Yu Zhu, Zhengrong Huang, Qiyuan Li, Weihua Li, Huiling Guo & Boan Li
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Catalog Antibody Subsequently, the membranes were incubated with HRP-conjugated secondary antibodies: Goat Anti-Rabbit IgG Antibody (GenScript, Cat#A00098) (dilution 1:5000), Goat Anti-Mouse IgG Antibody (GenScript, Cat#A00160) (dilution 1:5000) Get A Quote

摘要

Brown adipose tissue (BAT) is critical for non-shivering thermogenesis making it a promising therapeutic strategy to combat obesity and metabolic disease. However, the regulatory mechanisms underlying brown fat formation remain incompletely understood. Here, we found SOX4 is required for BAT development and thermogenic program. Depletion of SOX4 in BAT progenitors (Sox4-MKO) or brown adipocytes (Sox4-BKO) resulted in whitened BAT and hypothermia upon acute cold exposure. The reduced thermogenic capacity of Sox4-MKO mice increases their susceptibility to diet-induced obesity. Conversely, overexpression of SOX4 in BAT enhances thermogenesis counteracting diet-induced obesity. Mechanistically, SOX4 activates the t... More

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