CD146 Associates with Gp130 to Control a Macrophage Pro-inflammatory Program That Regulates the Metabolic Response to Obesity.
Hongxia DuanLin JingJianquan XiangChenhui JuZhenzhen WuJingyu LiuXinran MaXuehui ChenZheng LiuJing FengXiyun YanPublished in: Advanced science (Weinheim, Baden-Wurttemberg, Germany) (2022)
The mechanism of obesity-related metabolic dysfunction involves the development of systemic inflammation, largely mediated by macrophages. Switching of M1-like adipose tissue macrophages (ATMs) to M2-like ATMs, a population of macrophages associated with weight loss and insulin sensitivity, is considered a viable therapeutic strategy for obesity-related metabolic syndrome. However, mechanisms for reestablishing the polarization of ATMs remain elusive. This study demonstrates that CD146 + ATMs accumulate in adipose tissue during diet-induced obesity and are associated with increased body weight, systemic inflammation, and obesity-induced insulin resistance. Inactivating the macrophage CD146 gene or antibody targeting of CD146 alleviates obesity-related chronic inflammation and metabolic dysfunction. Macrophage CD146 interacts with Glycoprotein 130 (Gp130), the common subunit of the receptor signaling complex for the interleukin-6 family of cytokines. CD146/Gp130 interaction promotes pro-inflammatory polarization of ATMs by activating JNK signaling and inhibiting the activation of STAT3, a transcription factor for M2-like polarization. Disruption of their interaction by anti-CD146 antibody or interleukin-6 steers ATMs toward anti-inflammatory polarization, thus attenuating obesity-induced chronic inflammation and metabolic dysfunction in mice. The results suggest that macrophage CD146 is an important determinant of pro-inflammatory polarization and plays a pivotal role in obesity-induced metabolic dysfunction. CD146 could constitute a novel therapeutic target for obesity complications.
Keyphrases
- insulin resistance
- metabolic syndrome
- adipose tissue
- weight loss
- high fat diet induced
- type diabetes
- high fat diet
- oxidative stress
- weight gain
- skeletal muscle
- bariatric surgery
- transcription factor
- polycystic ovary syndrome
- roux en y gastric bypass
- nk cells
- diabetic rats
- body weight
- cardiovascular disease
- cell death
- high glucose
- copy number
- physical activity
- drug delivery
- mouse model