Author/Authors :
Keith D. Combrink، نويسنده , , H. Belgin Gulgeze، نويسنده , , Jan W. Thuring، نويسنده , , Kuo-Long Yu، نويسنده , , Rita L. Civiello، نويسنده , , Yi Zhang، نويسنده , , Bradley C. Pearce، نويسنده , , Zhiwei Yin، نويسنده , , David R. Langley، نويسنده , , Kathleen F. Kadow، نويسنده , , Christopher W. Cianci، نويسنده , , Zhufang Li، نويسنده , , Junius Clarke، نويسنده , , Eugene V. Genovesi، نويسنده , , Ivette Medina، نويسنده , , Lucinda Lamb، نويسنده , , Zheng Yang، نويسنده , , Lisa Zadjura، نويسنده , , Mark Krystal، نويسنده , , Nicholas A. Meanwell، نويسنده ,
Abstract :
The effect of structural variation of the benzimidazol-2-one ring of RSV fusion inhibitors related to BMS-433771 (1) was examined in conjunction with side chain modifications and the introduction of an aminomethyl substituent at the 5-position of the core benzimidazole moiety. Replacement of the benzimidazol-2-one moiety with benzoxazole, oxindole, quinoline-2-one, quinazolin-2,4-dione and benzothiazine derivatives provided a series of potent RSV fusion inhibitors 4. However, the intrinsic potency of 6,6-fused ring systems was generally less than that of comparably substituted 5,6-fused heterocycles of the type found in BMS-433771 (1). The introduction of an aminomethyl substituent to the benzimidazole ring enhanced antiviral activity in the 6,6-fused ring systems.
Keywords :
Respiratory syncytial virus inhibitors , RSV , RSV fusion inhibitors , antiviral agents , Benzimidazole derivatives
