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Hedgehog Partial Agonism Drives Warburg-like Metabolism in Muscle and Brown Fat
Author(s) -
Raffaele Teperino,
Sabine Amann,
Martina Bayer,
Sean L. McGee,
Andrea Loipetzberger,
Timothy Connor,
Carsten Jaeger,
Bernd Kammerer,
Lilli Winter,
Gerhard Wiche,
Kevin Dalgaard,
Madhan Selvaraj,
Michael Gaster,
Robert S. Lee,
Mark A. Febbraio,
Claude Knauf,
Patrice D. Cani,
Fritz Aberger,
Josef Penninger,
J. Andrew Pospisilik,
Harald Esterbauer
Publication year - 2012
Publication title -
cell
Language(s) - English
Resource type - Journals
SCImago Journal Rank - 26.304
H-Index - 776
eISSN - 1097-4172
pISSN - 0092-8674
DOI - 10.1016/j.cell.2012.09.021
Subject(s) - biology , agonism , smoothened , hedgehog , hedgehog signaling pathway , warburg effect , metabolism , microbiology and biotechnology , glycolysis , endocrinology , signal transduction , politics , political science , law
Diabetes, obesity, and cancer affect upward of 15% of the world's population. Interestingly, all three diseases juxtapose dysregulated intracellular signaling with altered metabolic state. Exactly which genetic factors define stable metabolic set points in vivo remains poorly understood. Here, we show that hedgehog signaling rewires cellular metabolism. We identify a cilium-dependent Smo-Ca(2+)-Ampk axis that triggers rapid Warburg-like metabolic reprogramming within minutes of activation and is required for proper metabolic selectivity and flexibility. We show that Smo modulators can uncouple the Smo-Ampk axis from canonical signaling and identify cyclopamine as one of a new class of "selective partial agonists," capable of concomitant inhibition of canonical and activation of noncanonical hedgehog signaling. Intriguingly, activation of the Smo-Ampk axis in vivo drives robust insulin-independent glucose uptake in muscle and brown adipose tissue. These data identify multiple noncanonical endpoints that are pivotal for rational design of hedgehog modulators and provide a new therapeutic avenue for obesity and diabetes.

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