Docking and Cytotoxicity Test on Human Breast Cancer Cell Line (T47d) of N-(Allylcarbamothioyl)-3-chlorobenzamide andN-(Allylcarbamothioyl)-3, 4-dichlorobenzamide

Siswandono and Tri Widiandani and Suko Hardjono (2017) Docking and Cytotoxicity Test on Human Breast Cancer Cell Line (T47d) of N-(Allylcarbamothioyl)-3-chlorobenzamide andN-(Allylcarbamothioyl)-3, 4-dichlorobenzamide. Research Journal of Pharmaceutical, Biological and Chemical Sciences, 8 (2). pp. 1909-1914. ISSN 0975-8585

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Official URL: https://www.rjpbcs.com/pdf/2017_8(2)/[209].pdf

Abstract

The specific objective of this research is to investigate the biological activity of thiourea derivativesby in silico study and the cytotoxicity test on human breast cancer cell lines. In this present study, the molecular docking of the new compound N-(allylcarbamothioyl)-3-chlorobenzamide (BATU-02) and N-(allylcarbamothioyl)-3,4-dichlorobenzamide (BATU-04) were evaluated on EGFR (1M17.pdb) using MVD v5.5 and showed that the re-rank scores of BATU-02 and BATU-04 are smaller than5-fluorouracil (5-FU). From the docking result, we can predict that the compounds have a higher biological activity. The cytotoxicity test were evaluated on human breast cancer cell lines (T47D) using MTT assay. Relevant result showed that these compounds(BATU-02 and BATU-04) demonstrated are more potent compared to 5-FU as the commercial anticancer drug, with respective IC50 were 128μg/mL (BATU-02); 86 μg/mL (BATU-04); and 213 μg/mL (5-FU).It can be concluded that the modification compounds of thiourea can be further developed as a potential anticancer drug.

Item Type: Article
Uncontrolled Keywords: Docking, thiourea, cytotoxicity, T47D, 1M17
Subjects: R Medicine
R Medicine > RS Pharmacy and materia medica
Divisions: 05. Fakultas Farmasi
Creators:
CreatorsNIM
SiswandonoNIDN0002105207
Tri WidiandaniNIDN0004128001
Suko HardjonoNIDN0028095204
Depositing User: Mr M. Fuad Sofyan
Date Deposited: 24 Jan 2020 02:05
Last Modified: 24 Jan 2020 02:05
URI: http://repository.unair.ac.id/id/eprint/93654
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