| Literature DB >> 16420067 |
Marco A Biamonte1, Jiandong Shi, Kevin Hong, David C Hurst, Lin Zhang, Junhua Fan, David J Busch, Patricia L Karjian, Angelica A Maldonado, John L Sensintaffar, Yong-Ching Yang, Adeela Kamal, Rachel E Lough, Karen Lundgren, Francis J Burrows, Gregg A Timony, Marcus F Boehm, Srinivas R Kasibhatla.
Abstract
Orally active Hsp90 inhibitors are of interest as potential chemotherapeutic agents. Recently, fully synthetic 8-benzyladenines and 8-sulfanyladenines such as 4 were disclosed as Hsp90 inhibitors, but these compounds are not water soluble and consequently have unacceptably low oral bioavailabilities. We now report that water-solubility can be achieved by inserting an amino functionality in the N(9) side chain. This results in compounds that are potent, soluble in aqueous media, and orally bioavailable. In an HER-2 degradation assay, the highest potency was achieved with the neopentylamine 42 (HER-2 IC(50) = 90 nM). In a murine tumor xenograft model (using the gastric cancer cell line N87), the H(3)PO(4) salts of the amines 38, 39, and 42 induced tumor growth inhibition when administered orally at 200 mg/kg/day. The amines 38, 39, and 42 are the first Hsp90 inhibitors shown to inhibit tumor growth upon oral dosage.Entities:
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Year: 2006 PMID: 16420067 DOI: 10.1021/jm0503087
Source DB: PubMed Journal: J Med Chem ISSN: 0022-2623 Impact factor: 7.446