| Literature DB >> 15956255 |
Yan Luo1, Alexander R Shoemaker, Xuesong Liu, Keith W Woods, Sheela A Thomas, Ron de Jong, Edward K Han, Tongmei Li, Vincent S Stoll, Jessica A Powlas, Anatol Oleksijew, Michael J Mitten, Yan Shi, Ran Guan, Thomas P McGonigal, Vered Klinghofer, Eric F Johnson, Joel D Leverson, Jennifer J Bouska, Mulugeta Mamo, Richard A Smith, Emily E Gramling-Evans, Bradley A Zinker, Amanda K Mika, Phong T Nguyen, Tilman Oltersdorf, Saul H Rosenberg, Qun Li, Vincent L Giranda.
Abstract
The Akt kinases are central nodes in signal transduction pathways that are important for cellular transformation and tumor progression. We report the development of a series of potent and selective indazole-pyridine based Akt inhibitors. These compounds, exemplified by A-443654 (K(i) = 160 pmol/L versus Akt1), inhibit Akt-dependent signal transduction in cells and in vivo in a dose-responsive manner. In vivo, the Akt inhibitors slow the progression of tumors when used as monotherapy or in combination with paclitaxel or rapamycin. Tumor growth inhibition was observed during the dosing interval, and the tumors regrew when compound administration was ceased. The therapeutic window for these compounds is narrow. Efficacy is achieved at doses approximately 2-fold lower than the maximally tolerated doses. Consistent with data from knockout animals, the Akt inhibitors induce an increase in insulin secretion. They also induce a reactive increase in Akt phosphorylation. Other toxicities observed, including malaise and weight loss, are consistent with abnormalities in glucose metabolism. These data show that direct Akt inhibition may be useful in cancer therapy, but significant metabolic toxicities are likely dose limiting.Entities:
Mesh:
Substances:
Year: 2005 PMID: 15956255 DOI: 10.1158/1535-7163.MCT-05-0005
Source DB: PubMed Journal: Mol Cancer Ther ISSN: 1535-7163 Impact factor: 6.261