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Targeting parvalbumin promotes M2 macrophage polarization and energy expenditure in mice.


ABSTRACT: Exercise benefits M2 macrophage polarization, energy homeostasis and protects against obesity partially through exercise-induced circulating factors. Here, by unbiased quantitative proteomics on serum samples from sedentary and exercised mice, we identify parvalbumin as a circulating factor suppressed by exercise. Parvalbumin functions as a non-competitive CSF1R antagonist to inhibit M2 macrophage activation and energy expenditure in adipose tissue. More importantly, serum concentrations of parvalbumin positively correlate with obesity in mouse and human, while treating mice with a recombinant parvalbumin blocker prevents its interaction with CSF1R and promotes M2 macrophage polarization and ameliorates diet-induced obesity. Thus, although further studies are required to assess the significance of parvalbumin in mediating the effects of exercise, our results implicate parvalbumin as a potential therapeutic strategy against obesity in mice.

SUBMITTER: Lin S 

PROVIDER: S-EPMC9177846 | biostudies-literature | 2022 Jun

REPOSITORIES: biostudies-literature

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Targeting parvalbumin promotes M2 macrophage polarization and energy expenditure in mice.

Lin Shaojian S   Zhang Anke A   Yuan Ling L   Wang Yufan Y   Zhang Chuan C   Jiang Junkun J   Xu Houshi H   Yuan Huiwen H   Yao Hui H   Zhang Qianying Q   Zhang Yong Y   Lou Meiqing M   Wang Ping P   Zhang Zhen-Ning ZN   Luan Bing B  

Nature communications 20220608 1


Exercise benefits M2 macrophage polarization, energy homeostasis and protects against obesity partially through exercise-induced circulating factors. Here, by unbiased quantitative proteomics on serum samples from sedentary and exercised mice, we identify parvalbumin as a circulating factor suppressed by exercise. Parvalbumin functions as a non-competitive CSF1R antagonist to inhibit M2 macrophage activation and energy expenditure in adipose tissue. More importantly, serum concentrations of parv  ...[more]

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