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Nitric oxide releasing acridone carboxamide derivatives as reverters of doxorubicin resistance in MCF7/Dx cancer cells
Institution:1. Centre for Chemical Sciences and Technology, Institute of Science and Technology, Jawaharlal Nehru Technological University Hyderabad, Hyderabad, Telangana 500085, India;2. Discovery Chemistry Solutions, Aragen Life Sciences Pvt. Ltd (formerly called as GVK Biosciences Private Limited), Plot No. 284 Part A, Bommasandra Jigani Link Road, Jigani, Bengaluru, Karnataka 562106, India;3. Department of Chemistry, Veer Surendra Sai University of Technology, Burla-768018, Odisha, India;1. Institute of Medical Biology, Polish Academy of Sciences, Lodz, Poland;2. Department of Gynecology and Gynecologic Oncology, Polish Mother''s Memorial Hospital—Research Institute, Lodz, Poland
Abstract:A series of nitric oxide donating acridone derivatives are synthesized and evaluated for in vitro cytotoxic activity against different sensitive and resistant cancer cell lines MCF7/Wt, MCF7/Mr (BCRP overexpression) and MCF7/Dx (P-gp expression). The results showed that NO-donating acridones are potent against both the sensitive and resistant cells. Structure activity relationship indicate that the nitric oxide donating moiety connected through a butyl chain at N10 position as well as morpholino moiety linkage through an amide bridge on the acridone ring system at C-2 position, are required to exert a good cytotoxic effect. Further, good correlations were observed when cytotoxic properties were compared with in vitro nitric oxide release rate, nitric oxide donating group potentiated the cytotoxic effect of the acridone derivatives. Exogenous release of nitric oxide by NO donating acridones enhanced the accumulation of doxorubicin in MCF7/Dx cell lines when it was coadministered with doxorubicin, which inhibited the efflux process of doxorubicin. In summary, a nitric oxide donating group can potentiate the anti-MDR property of acridones.
Keywords:Nitric oxide  Acridone  Doxorubicin  Breast cancer
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