Immunoglobulin G (IgG) is traditionally recognized as a plasma protein that neutralizes antigens for immune defense. However, our research demonstrates that IgG predominantly accumulates in adipose tissue during obesity development, triggering insulin resistance and macrophage infiltration. This accumulation is governed by neonatal Fc receptor (FcRn)-dependent recycling, orchestrated in adipose progenitor cells and macrophages during the early and late stages of diet-induced obesity (DIO), respectively. Targeting FcRn abolished IgG accumulation and rectified insulin resistance and metabolic degeneration in DIO. By integrating artificial intelligence (AI) modeling with in vivo and in vitro experimental models, we unexpectedly uncovered an interaction between IgG's Fc-CH3 domain and the insulin receptor's ectodomain. This interaction hinders insulin binding, consequently obstructing insulin signaling and adipocyte functions. These findings unveil adipose IgG accumulation as a driving force in obesity pathophysiology, providing a novel therapeutic strategy to tackle metabolic dysfunctions.
FcRn-dependent IgG accumulation in adipose tissue unmasks obesity pathophysiology.
脂肪组织中 FcRn 依赖性 IgG 的积累揭示了肥胖的病理生理机制
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作者:Yu Lexiang, Yang Yong Xiao, Gong Zhen, Wan Qianfen, Du Yifei, Zhou Qiuzhong, Xiao Yang, Zahr Tarik, Wang Zhaobin, Yu Zhewei, Yang Kangkang, Geng Jinyang, Fried Susan K, Li Jing, Haeusler Rebecca A, Leong Kam W, Bai Lin, Wu Yingjie, Sun Lei, Wang Pan, Zhu Bao Ting, Wang Liheng, Qiang Li
| 期刊: | Cell Metabolism | 影响因子: | 30.900 |
| 时间: | 2025 | 起止号: | 2025 Mar 4; 37(3):656-672 |
| doi: | 10.1016/j.cmet.2024.11.001 | 靶点: | IgG |
| 研究方向: | 信号转导 | ||
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