Author/Authors :
Renee N. Brown، نويسنده , , Rachel Cameron، نويسنده , , David K. Chalmers، نويسنده , , Stephanie Hamilton، نويسنده , , Angela Luttick، نويسنده , , Guy Y. Krippner، نويسنده , , Darryl B. McConnell، نويسنده , , Roland Nearn، نويسنده , , Pauline C. Stanislawski، نويسنده , , Simon P. Tucker، نويسنده , , Keith G. Watson، نويسنده ,
Abstract :
A series of pyridazinylpiperidinyl capsid-binding compounds with novel bicyclic substituents were synthesized and screened against human rhinovirus (HRV). Several 2-alkoxy- and 2-alkylthio-benzoxazole and benzothiazole derivatives showed excellent anti-HRV activity. When tested against a panel of 16 representative HRV types the 2-ethoxybenzoxazole derivative 13 was found to have superior HRV activity (median EC50 3.88 ng/mL) to known capsid-binders Pleconaril and Pirodavir. Compound 13 illustrates that a 2-alkoxybenzoxazole group can be an effective bioisostere for a benzoate ester or benzaldehyde oxime ether functionality.
Keywords :
Bioisostere , Benzoxazole , Rhinovirus , HRV , antiviral
