| Article ID | Journal | Published Year | Pages | File Type |
|---|---|---|---|---|
| 2040662 | Cell Reports | 2015 | 8 Pages |
•We identify eggmanone from an in vivo chemical genetic screen•Eggmanone inhibits Hedgehog signaling through phosphodiesterase 4 antagonism•Eggmanone targets Hedgehog signaling downstream of Smoothened•Eggmanone defines a strategy for treatment of Hedgehog-dependent cancers
SummaryHedgehog (Hh) signaling plays an integral role in vertebrate development, and its dysregulation has been accepted widely as a driver of numerous malignancies. While a variety of small molecules target Smoothened (Smo) as a strategy for Hh inhibition, Smo gain-of-function mutations have limited their clinical implementation. Modulation of targets downstream of Smo could define a paradigm for treatment of Hh-dependent cancers. Here, we describe eggmanone, a small molecule identified from a chemical genetic zebrafish screen, which induced an Hh-null phenotype. Eggmanone exerts its Hh-inhibitory effects through selective antagonism of phosphodiesterase 4 (PDE4), leading to protein kinase A activation and subsequent Hh blockade. Our study implicates PDE4 as a target for Hh inhibition, suggests an improved strategy for Hh-dependent cancer therapy, and identifies a unique probe of downstream-of-Smo Hh modulation.
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