Molecular Docking Studies of a Chalcone Derivative Compound p-hydroxy-m-methoxychalcone with Tyrosine Kinase Receptors

Indian Journal of Public Health Research & Development
Year : 2019, Volume : 10, Issue : 7
First page : ( 1219) Last page : ( 1224)
Print ISSN : 0976-0245. Online ISSN : 0976-5506.
Article DOI : 10.5958/0976-5506.2019.01752.2

Arianingrum Retno^1,^3,*, Hermawan Adam^2,³, Purnomo Hari^2,³, Dewi Dyaningtyas^2,³, Meiyanto Edy^2,³

¹Department of Chemistry Education, Universitas Negeri Yogyakarta, Indonesia

²Faculty of Pharmaceutical, Universitas Gadjah Mada, Indonesia

³Cancer Chemoprevention Research Center, Universitas Gadjah Mada, Indonesia

*Corresponding Author: Retno Arianingrum, Department of Chemistry Education, Universitas Negeri Yogyakarta, Indonesia Email: Arianingrum@uny.ac.id

Online published on 19 August, 2019.

Abstract

Chalcone compounds have been studied as therapeutic, especially as antitumor drugs. A chalcone derivate, para-hydroxy-metha-methoxychalcone (pHmMC) or 3-(4’-hydroxy-3’-methoxyphenyl)-1-phenyl-2propene-1-on, has been studied to explore its potential utilization as chemoprevention in several cancers cell lines. The main objective of the present work is to perform a docking analysis of pHmMC with tyrosine kinase receptors EGFR, HER2, and VEGFR comparing with ligand ATP. Docking studies were performed using PLANTS (Protein Ligand ANT System) software, while the preparations of protein and reference ligand was used YASARA, and visualizing amino acids was used Molecular Operating Environment (MOE) program. The docking studies indicated that the binding energy of pHmMC with EGFR (1XKK) and HER2 (3PPO) was higher than the ATP binding energy with the EGFR and HER2. However, the binding energy of pHmMC with VEGFR (2P2I) almost had the same energy binding compared with the ATP binding on VEGFR. VEGF is a protein that plays a role in angiogenesis. Data from the MOE program showed there were similarities in the amino acids involved in the interaction between pHmMC and ATP in binding to EGFR, HER2, and VEGFR. The results indicated that pHmMC has the potential to be developed as an anticancer which might through the mechanism of inhibiting the process of angiogenesis.

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Keywords

Molecular docking, pHmMC, EGFR, HER2, VEGFR.

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