MondoA coordinately regulates skeletal myocyte lipid homeostasis and insulin signaling
Byungyong Ahn, … , Rick B. Vega, Daniel P. Kelly
Byungyong Ahn, … , Rick B. Vega, Daniel P. Kelly
Published August 8, 2016
Citation Information: J Clin Invest. 2016;126(9):3567-3579. https://doi.org/10.1172/JCI87382.
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MondoA coordinately regulates skeletal myocyte lipid homeostasis and insulin signaling

Abstract

Intramuscular lipid accumulation is a common manifestation of chronic caloric excess and obesity that is strongly associated with insulin resistance. The mechanistic links between lipid accumulation in myocytes and insulin resistance are not completely understood. In this work, we used a high-throughput chemical biology screen to identify a small-molecule probe, SBI-477, that coordinately inhibited triacylglyceride (TAG) synthesis and enhanced basal glucose uptake in human skeletal myocytes. We then determined that SBI-477 stimulated insulin signaling by deactivating the transcription factor MondoA, leading to reduced expression of the insulin pathway suppressors thioredoxin-interacting protein (TXNIP) and arrestin domain–containing 4 (ARRDC4). Depleting MondoA in myocytes reproduced the effects of SBI-477 on glucose uptake and myocyte lipid accumulation. Furthermore, an analog of SBI-477 suppressed TXNIP expression, reduced muscle and liver TAG levels, enhanced insulin signaling, and improved glucose tolerance in mice fed a high-fat diet. These results identify a key role for MondoA-directed programs in the coordinated control of myocyte lipid balance and insulin signaling and suggest that this pathway may have potential as a therapeutic target for insulin resistance and lipotoxicity.

Authors

Byungyong Ahn, Mangala M. Soundarapandian, Hampton Sessions, Satyamaheshwar Peddibhotla, Gregory P. Roth, Jian-Liang Li, Eliot Sugarman, Ada Koo, Siobhan Malany, Miao Wang, Kyungmoo Yea, Jeanne Brooks, Teresa C. Leone, Xianlin Han, Rick B. Vega, Daniel P. Kelly

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Figure 1

SBI-477 is a small-molecule inhibitor of neutral lipid accumulation in human skeletal myotubes.

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SBI-477 is a small-molecule inhibitor of neutral lipid accumulation in h...
(A) Chemical structure of SBI-477. (B) Effects of SBI-477, over a dose range, on triglyceride levels in human skeletal myotubes following a 24-hour exposure to 100 μM oleate. Data are shown as the percentage of DMSO vehicle control and are representative of more than 5 experiments. (C) Effects of SBI-477 on human skeletal myotube neutral lipid accumulation as visualized by AdipoRed staining (red). Cell nuclei were stained with DAPI (blue). Images shown are representative of more than 3 images.