1. In VitroAntiviral Characteristics of HIV-1 Attachment Inhibitor BMS-626529, the Active Component of the Prodrug BMS-663068
- Author
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Nowicka-Sans, Beata, Gong, Yi-Fei, McAuliffe, Brian, Dicker, Ira, Ho, Hsu-Tso, Zhou, Nannan, Eggers, Betsy, Lin, Pin-Fang, Ray, Neelanjana, Wind-Rotolo, Megan, Zhu, Li, Majumdar, Antara, Stock, David, Lataillade, Max, Hanna, George J., Matiskella, John D., Ueda, Yasutsugu, Wang, Tao, Kadow, John F., Meanwell, Nicholas A., and Krystal, Mark
- Abstract
ABSTRACTBMS-663068 is the phosphonooxymethyl prodrug of BMS-626529, a novel small-molecule attachment inhibitor that targets HIV-1 gp120 and prevents its binding to CD4+T cells. The activity of BMS-626529 is virus dependent, due to heterogeneity within gp120. In order to better understand the anti-HIV-1 spectrum of BMS-626529 against HIV-1, in vitroactivities against a wide variety of laboratory strains and clinical isolates were determined. BMS-626529 had half-maximal effective concentration (EC50) values of <10 nM against the vast majority of viral isolates; however, susceptibility varied by >6 log10, with half-maximal effective concentration values in the low pM range against the most susceptible viruses. The in vitroantiviral activity of BMS-626529 was generally not associated with either tropism or subtype, with few exceptions. Measurement of the binding affinity of BMS-626529 for purified gp120 suggests that a contributory factor to its inhibitory potency may be a relatively long dissociative half-life. Finally, in two-drug combination studies, BMS-626529 demonstrated additive or synergistic interactions with antiretroviral drugs of different mechanistic classes. These results suggest that BMS-626529 should be active against the majority of HIV-1 viruses and support the continued clinical development of the compound.
- Published
- 2012
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