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Discovery and SAR exploration of |
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| Authors: | Mikhail Krasavin Konstantin A Rufanov Andrey V Sosnov Ruben Karapetian Elena Godovykh Olga Soldatkina Yan Lavrovsky Andrei A Gakh |
| Affiliation: | (1) Department of Medicinal Chemistry, Chemical Diversity Research Institute, 2a Rabochaya St, 141400 Khimki, Moscow Reg, Russian Federation;(2) Innovation Department, Chemical Diversity Research Institute, 2a Rabochaya St, 141400 Khimki, Moscow Reg, Russian Federation;(3) Department of Lead Discovery, Chemical Diversity Research Institute, 2a Rabochaya St, 141400 Khimki, Moscow Reg, Russian Federation;(4) Oak Ridge National Laboratory, Bethel Valley Rd, 37831-6242 Oak Ridge, TN, USA |
| Abstract: | A new chemical series of antiproliferative compounds was identified via high-throughput screening on DU-145 human prostate carcinoma cell line (hit compound potency - 5.7 μM). Exploration of the two peripheral diversity vectors of the hit molecule in a hit-targeted library and testing of the resulting compounds led to SAR generalizations and identification of the 'best' pharmacophoric moieties. The latter were merged in a single compound that exhibited a 200-fold better potency than the original hit compound. Specific cancer cell cytotoxicity was confirmed for the most potent compounds. |
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