Evaluation of a multi-kinase inhibitor KRC-108 as an anti-tumor agent in vitro and in vivo |
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Authors: | Sun-Young Han Chong Ock Lee Sung-Hoon Ahn Mi-Ok Lee So-Young Kang Hyuk-Jin Cha Sung Yun Cho Jae Du Ha Jae Wook Ryu Heejung Jung Hyoung Rae Kim Jong Sung Koh Jongkook Lee |
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Affiliation: | 1. Bio-Organic Science Division, Korea Research Institute of Chemical Technology, PO Box?107, Yuseong, Daejeon, 305-600, Korea 4. College of Pharmacy and Institute of Health Sciences, Gyeongsang National University, Jinju, 660-751, Korea 2. Department of Biomedical Science, College of Life Science, CHA University, Pochon-si, Gyeonggi-do, 487-801, Korea 3. Stem Cell Research Laboratory, CHA Stem Cell Institute, CHA University, Seoul, 135-907, Korea
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Abstract: | Kinases have been studied as potential cancer targets because they play important roles in the cellular signaling of tumors. A number of small molecules targeting kinases are prescribed in clinics and many kinase inhibitors are being evaluated in the clinical phase. Previously, we discovered a series of aminopyridines substituted with benzoxazole as orally active c-Met kinase inhibitors. One of the compounds, KRC-108, has been evaluated as an anti-cancer agent in vitro and in vivo. A kinase panel assay exhibited that KRC-108 is a potent inhibitor of Ron, Flt3 and TrkA as well as c-Met. Moreover, KRC-108 inhibited oncogenic c-Met M1250T and Y1230D more strongly than wild type c-Met. The anti-proliferative activity of KRC-108 was measured by performing a cytotoxicity assay on a panel of cancer cell lines. The GI(50) values (i.e., 50% inhibition of cell growth) for KRC-108 ranged from 0.01 to 4.22?μM for these cancer cell lines. KRC-108 was also effective for the inhibition of tumor growth in human HT29 colorectal cancer and NCI-H441 lung cancer xenograft models in athymic BALB/c nu/nu mice. This molecule should serve as a useful lead for inhibitors targeting kinases and may lead to new therapeutics for the treatment of cancer. |
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