| Literature DB >> 19035287 |
Joann P Palma1, Luis E Rodriguez, Velitchka D Bontcheva-Diaz, Jennifer J Bouska, Gail Bukofzer, Milagros Colon-Lopez, Ran Guan, Kenneth Jarvis, Eric F Johnson, Vered Klinghofer, Xuesong Liu, Amanda Olson, Mary J Saltarelli, Yan Shi, Jason A Stavropoulos, Gui-Dong Zhu, Thomas D Penning, Yan Luo, Vincent L Giranda, Saul H Rosenberg, David J Frost, Cherrie K Donawho.
Abstract
ABT-888 is a potent, orally bioavailable PARP-1/2 inhibitor shown to potentiate DNA damaging agents. The ability to potentiate temozolomide (TMZ) and develop a biological marker for PARP inhibition was evaluated in vivo. Doses/schedules that achieve TMZ potentiation in the B16F10 syngeneic melanoma model were utilized to develop an ELISA to detect a pharmacodynamic marker, ADP ribose polymers (pADPr), after ABT 888 treatment. ABT-888 enhanced TMZ antitumor activity, in a dose-proportional manner with no observed toxicity (44-75% tumor growth inhibition vs. TMZ monotherapy), but did not show single agent activity. Extended ABT-888 dosing schedules showed no advantage compared to simultaneous TMZ administration. Efficacy correlated with plasma/tumor drug concentrations. Intratumor drug levels correlated with a dose-proportional/time-dependent reduction in pADPr. Potentiation of TMZ activity by ABT-888 correlated with drug levels and inhibition of PARP activity in vivo. ABT-888 is in Phase 1 trials using a validated ELISA based on the assay developed here to assess pharmacological effect.Entities:
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Year: 2008 PMID: 19035287
Source DB: PubMed Journal: Anticancer Res ISSN: 0250-7005 Impact factor: 2.480