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Sympathetic neuropeptide Y protects from obesity by sustaining thermogenic fat.

Nature (2024-08-31)
Yitao Zhu, Lu Yao, Ana L Gallo-Ferraz, Bruna Bombassaro, Marcela R Simões, Ichitaro Abe, Jing Chen, Gitalee Sarker, Alessandro Ciccarelli, Linna Zhou, Carl Lee, Davi Sidarta-Oliveira, Noelia Martínez-Sánchez, Michael L Dustin, Cheng Zhan, Tamas L Horvath, Licio A Velloso, Shingo Kajimura, Ana I Domingos
要旨

Human mutations in neuropeptide Y (NPY) have been linked to high body mass index but not altered dietary patterns1. Here we uncover the mechanism by which NPY in sympathetic neurons2,3 protects from obesity. Imaging of cleared mouse brown and white adipose tissue (BAT and WAT, respectively) established that NPY+ sympathetic axons are a smaller subset that mostly maps to the perivasculature; analysis of single-cell RNA sequencing datasets identified mural cells as the main NPY-responsive cells in adipose tissues. We show that NPY sustains the proliferation of mural cells, which are a source of thermogenic adipocytes in both BAT and WAT4-6. We found that diet-induced obesity leads to neuropathy of NPY+ axons and concomitant depletion of mural cells. This defect was replicated in mice with NPY abrogated from sympathetic neurons. The loss of NPY in sympathetic neurons whitened interscapular BAT, reducing its thermogenic ability and decreasing energy expenditure before the onset of obesity. It also caused adult-onset obesity of mice fed on a regular chow diet and rendered them more susceptible to diet-induced obesity without increasing food consumption. Our results indicate that, relative to central NPY, peripheral NPY produced by sympathetic nerves has the opposite effect on body weight by sustaining energy expenditure independently of food intake.

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Sigma-Aldrich
抗チロシンヒドロキシラーゼ抗体, Chemicon®, from rabbit
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抗アクチン, α-平滑筋 - Cy3抗体, マウスモノクロナール, clone 1A4, purified from hybridoma cell culture
Sigma-Aldrich
Anti-NG2 Antibody, clone 132.39, Alexa Fluor488 Conjugate, clone 132.39, from mouse, ALEXA FLUOR 488