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Synthesis of 2-Fluoro N10-Substituted Acridones and Their Cytotoxicity Studies in Sensitive and Resistant Cancer Cell Lines and Their DNA Intercalation Studies
Authors:Yergeri C. Mayur  Zaheeruddin  Godefridus J. Peters  Clara Lemos  Ietje Kathmann  Velivela V. S. Rajendra Prasad
Affiliation:1. Medicinal Chemistry Research Devision, V. L. College of Pharmacy, Raichur, India. Tel/Fax: +91 8532 240-405;2. Department of Medical Oncology, VU University Medical Center, Amsterdam, The Netherlands;3. Department of Medical Oncology, VU University Medical Center, Amsterdam, The Netherlands

Department of Biochemistry (U38-FCT), Faculty of Medicine, University of Porto, Porto, Portugal

Abstract:A series of 2-fluoro N10-substituted acridone derivatives with varying alkyl side chain length with propyl, butyl substitution, and a tertiary amine group at the terminal end of the alkyl side chain were synthesized and screened against cancer cell lines SW 1573, SW 1573 2R 160 (P-gp substrate) which are non-small lung cancer cell lines, MCF-7, MCF-7/MR (BCRP substrate) are breast cancer cell lines, 2008 WT, 2008MRP1, 2008MRP2, 2008MRP3 are ovarian cancer cell lines, and human embryo kidney cell lines like HEK293, HEK293 MRP4, and HEK293 MRP5i. The propyl-series compounds showed lipophilicity in the range of 1.93 to 4.40 and the butyl series in the range of 2.37 to 4.78. The compounds 4 , 7 , and 8 showed good cytotoxicity against the 60 human cancer cell line panel of the National Cancer Institute, USA. The compounds 14 and 15 showed a better cytotoxicity in most of the cancer cell lines compared to other compounds tested. The DNA-binding properties of the compounds were evaluated based on their affinity or intercalation with CT-DNA measured with absorption titration. The compound 11 bearing planar tricyclic ring linked with a butyl methylpiperazino side chain showed the highest binding affinity with a binding constant (Ki) of 10.38×10 M–1. Evaluation of the compounds in cell lines with an overexpression of various multidrug resistance-related protein (MRP), P-glycoprotein (P-gp), or Breast Cancer Resistance Protein (BCRP) showed that all compounds are not substrates for any of these transporters.
Keywords:Acridone  Mitoxantrone  Multidrug resistance (MDR)  P-glycoprotein
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