Novel Antitumor L‐Arabinose Derivative of Indolocarbazole with High Affinity to DNA |
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| Authors: | Dmitry N. Kaluzhny Dr. Victor V. Tatarskiy Jr. Lyubov G. Dezhenkova Dr. Irina L. Plikhtyak Dr. Tatyana D. Miniker Dr. Anna K. Shchyolkina Dr. Sergey A. Strel'tsov Dr. Ghermes G. Chilov Dr. Fedor N. Novikov Dr. Irina Yu. Kubasova Dr. Zoya S. Smirnova Dr. Stalina Ya. Mel'nik Dr. Mikhail A. Livshits Dr. Olga F. Borisova Dr. Alexander A. Shtil Dr. |
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| Affiliation: | 1. Engelhardt Institute of Molecular Biology, 32 Vavilov Street, Moscow 119991 (Russian Federation), Fax: (+7)?499‐135‐1405;2. Blokhin Cancer Center, 24 Kashirskoye shosse, Moscow 115478 (Russian Federation), Fax: (+7)?495‐324‐1205;3. Gause Institute of New Antibiotics, 11?B. Pirogovskaya Street, Moscow 119021 (Russian Federation);4. MolTech, Ltd., 1/75A Leninskie Gory, Moscow 119992 (Russian Federation) |
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| Abstract: | Novel indolocarbazole derivative 12‐(α‐L ‐arabinopyranosyl)indolo[2,3‐α]pyrrolo[3,4‐c]carbazole‐5,7‐dione (AIC) demonstrated high potency (at submicromolar concentrations) against the NCI panel of human tumor cell lines and transplanted tumors in vivo. In search of tentative targets for AIC, we found that the drug formed high affinity intercalative complexes with d(AT)20, d(GC)20 and calf thymus DNA (binding constants (1.6×106) M ?1≤Ka≤(3.3×106) M ?1). The drug intercalated preferentially into GC pairs of the duplex. Importantly, the concentrations at which AIC formed the intercalative complexes with DNA (C≤1 μM ) were identical to the concentrations that triggered p53‐dependent gene reporter transactivation, the replication block, the inhibition of topoisomerase I‐mediated DNA relaxation and death of HCT116 human colon carcinoma cells. We conclude that the formation of high affinity intercalative complexes with DNA is an important factor for anticancer efficacy of AIC. |
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| Keywords: | antitumor agents binding constants DNA indolocarbazoles intercalation |
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