Discovery of 4-Hydroxy-3-(3-(phenylureido)benzenesulfonamides as SLC-0111 Analogues for the Treatment of Hypoxic Tumors Overexpressing Carbonic Anhydrase IX.
Murat BozdagFabrizio CartaMariangela CerusoMarta FerraroniPaul C McDonaldShoukat DedharClaudiu T SupuranPublished in: Journal of medicinal chemistry (2018)
Herein we report the 2-aminophenol-4-sulfonamide 1 and its ureido derivatives 2-23 as inhibitors of the carbonic anhydrase (CA, EC 4.2.1.1) enzymes as analogues of the hypoxic tumor phase II entering drug SLC-0111. This scaffold may determine preferential rotational isomers to selectively interact within the tumor-associated CAs. Most of the compounds indeed showed in vitro selective inhibition of the tumor associated CA isoforms IX and XII. The most potent derivative within the series was 11 ( KIs of 2.59 and 7.64 nM on hCA IX and XII, respectively), which shares the 4-fluorophenylureido tail with the clinical candidate. We investigated by means of X-ray crystallographic studies the binding modes of three selected compounds of this series to CA I. The evaluation of therapeutic efficacy of compound 11 in an orthotopic, syngeneic model of CA IX-positive breast cancer in vivo showed close matching antitumoral effects and tolerance with SLC-0111.
Keyphrases
- phase ii
- positive breast cancer
- clinical trial
- protein kinase
- molecular docking
- open label
- small molecule
- crispr cas
- high resolution
- photodynamic therapy
- high throughput
- randomized controlled trial
- computed tomography
- magnetic resonance
- combination therapy
- structure activity relationship
- drug induced
- case control
- study protocol
- double blind
- single cell