Synthesis, and  Anti-Tumor Evaluation of Some New Flurbiprofen  Derivatives Against MCF-7  and WRL-68 Cell Lines

Kasim S. Hmood; Ammar A. Razzak  Mahmood  Kubba; Redha  I Al-bayati; Abdulrahman M.  Saleh

doi:10.22146/ijp.730

Indonesian Journal of Pharmacy (Jan 2021)

Synthesis, and Anti-Tumor Evaluation of Some New Flurbiprofen Derivatives Against MCF-7 and WRL-68 Cell Lines

Kasim S. Hmood,
Ammar A. Razzak Mahmood Kubba,
Redha I Al-bayati,
Abdulrahman M. Saleh

Affiliations

Kasim S. Hmood: Iraqi Ministry of Health, Wasit Health Directorate- Department of Pharmacy, Wasit-Iraq
Ammar A. Razzak Mahmood Kubba: Department of Pharmaceutical Chemistry, College of Pharmacy-University of Baghdad, Baghdad, Bab-Al-Mouadam-10001-Iraq
Redha I Al-bayati: Department of Chemistry, College of Science, Al-Mustansirya University, Baghdad, 10001, Iraq
Abdulrahman M. Saleh: Pharmaceutical Medicinal Chemistry and Drug Design Department, Faculty of Pharmacy (Boys), Al-Azhar University. Cairo 11884, Egypt

DOI: https://doi.org/10.22146/ijp.730

Abstract

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A new series of flurbiprofen derivatives containing thiosemicarbazide moiety (3-7) was synthesized from flurbiprofen as parent nucleus by esterification, hydrazide formation, and heating with different aryl isothiocyanate substituents, respectively. Flurbiprofen was also treated with thiosemicarbazide in the presence POCl3 as a catalyst, to produce 1,3,4 -thiadiazole -2-amine (8). Treatment of (8) with different aryl isothiocyanates produced thiourea derivatives (9-12). Also, the reaction of (8) with different benzoyl chloride substituents produced benzamide compounds (13-15). Eventually , treatment of (8) with ethyl acetoacetate(EAA) produced [1,3,4]thiadiazolo[3,2-a]pyrimidin-7-one (16) .The new compounds were characterized by spectroscopic techniques :FTIR, 1HNMR, and CHNS analysis. A molecular docking study for the synthesized compounds (3-16), against the Vascular Endothelial Growth Factor receptor (VEGFR-2) was applied and it indicated that compounds 4,7,13, and 15,exhibited the optimum binding energy of -6.77, -6.12,-6.68, and -6.43 kcal/mol, respectively. Target compounds were also assessed for their in vitro anticancer effects in a cell-line study. All of the compounds tested showed the most plausible anticancer activity, compared to a positive control(Sorafenib), using in vitro MTT cytotoxic assay ,against human breast tumor (MCF-7), and normal WRL-68 cell line. The in vitro results revealed that compounds 4,5,10,11,13, and 15 exhibited the highest inhibitory activity at their IC50 concentrations, against MCF-7 cell lines, as follows (122.7,113.9,95,7. 109.1,40.32 and 112.29µg/mL, respectively. While their cytotoxic effect against normal WRL-68 cell line at their IC50 concentrations, as follow 210.2, 181.3 ,151.7,278.7,80.28, and 236 µg/mL, respectively, therefore, such compounds were considered more selective toward MCF-7 than normal WRL-68,and their selectivity index (SI): 1.71,1.59,1.59 ,2.55 ,1.99 , and 2.10,respectively . Among the synthesized compounds, the compound 15 was chosen to screen its effect in vitro through multi-parameter cytotoxic assay against MCF-7 breast cancer implemented in High Content Screening (ArrayScan XTI, Thermo Scientific),which could be taken in consideration as a starting point for the development of new anticancer drugs

Published in Indonesian Journal of Pharmacy

ISSN: 2338-9427 (Print); 2338-9486 (Online)
Publisher: Universitas Gadjah Mada
Country of publisher: Indonesia
LCC subjects: Medicine: Pharmacy and materia medica
Website: https://jurnal.ugm.ac.id/v3/IJP

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