Brown Adipose Tissue Controls Skeletal Muscle Function via the Secretion of Myostatin

棕色脂肪组织通过分泌肌生长抑制素来控制骨骼肌功能

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作者：Xingxing Kong, Ting Yao, Peng Zhou, Lawrence Kazak, Danielle Tenen, Anna Lyubetskaya, Brian A Dawes, Linus Tsai, Barbara B Kahn, Bruce M Spiegelman, Tiemin Liu, Evan D Rosen

期刊：

Cell Metabolism

影响因子：

27.700

时间：

2018

起止号：

2018 Oct 2;28(4):631-643.e3.

doi：

10.1016/j.cmet.2018.07.004

研究方向：

信号转导

Abstract

Skeletal muscle and brown adipose tissue (BAT) are functionally linked, as exercise increases browning via secretion of myokines. It is unknown whether BAT affects muscle function. Here, we find that loss of the transcription factor IRF4 in BAT (BATI4KO) reduces exercise capacity, mitochondrial function, ribosomal protein synthesis, and mTOR signaling in muscle and causes tubular aggregate formation. Loss of IRF4 induces myogenic gene expression in BAT, including the secreted factor myostatin, a known inhibitor of muscle function. Reducing myostatin via neutralizing antibodies or soluble receptor rescues the exercise capacity of BATI4KO mice. In addition, overexpression of IRF4 in brown adipocytes reduces serum myostatin and increases exercise capacity in muscle. Finally, mice housed at thermoneutrality have reduced IRF4 in BAT, lower exercise capacity, and elevated serum myostatin; these abnormalities are corrected by excising BAT. Collectively, our data point to an unsuspected level of BAT-muscle crosstalk driven by IRF4 and myostatin.

Brown Adipose Tissue Controls Skeletal Muscle Function via the Secretion of Myostatin

棕色脂肪组织通过分泌肌生长抑制素来控制骨骼肌功能

Abstract

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