A New Smoothened Antagonist Bearing the Purine Scaffold Shows Antitumour Activity In Vitro and In Vivo.
Ana María ZarateChristian Espinosa-BustosSimón GuerreroAngélica FierroFelipe Oyarzún-AmpueroAndrew Frederick Geoffery QuestLucia Di MarcotullioElena LoricchioMiriam CaimanoAndrea CalcaterraMatías González-QuirozAdam AguirreJaime MeléndezCristian O SalasPublished in: International journal of molecular sciences (2021)
The Smoothened (SMO) receptor is the most druggable target in the Hedgehog (HH) pathway for anticancer compounds. However, SMO antagonists such as vismodegib rapidly develop drug resistance. In this study, new SMO antagonists having the versatile purine ring as a scaffold were designed, synthesised, and biologically tested to provide an insight to their mechanism of action. Compound 4s was the most active and the best inhibitor of cell growth and selectively cytotoxic to cancer cells. 4s induced cell cycle arrest, apoptosis, a reduction in colony formation and downregulation of PTCH and GLI1 expression. BODIPY-cyclopamine displacement assays confirmed 4s is a SMO antagonist. In vivo, 4s strongly inhibited tumour relapse and metastasis of melanoma cells in mice. In vitro, 4s was more efficient than vismodegib to induce apoptosis in human cancer cells and that might be attributed to its dual ability to function as a SMO antagonist and apoptosis inducer.
Keyphrases
- cell cycle arrest
- cell death
- pi k akt
- basal cell carcinoma
- signaling pathway
- endoplasmic reticulum stress
- oxidative stress
- endothelial cells
- cell proliferation
- poor prognosis
- high glucose
- high throughput
- type diabetes
- adipose tissue
- drug induced
- fluorescent probe
- high fat diet induced
- insulin resistance
- metabolic syndrome
- single molecule
- single cell
- anti inflammatory