Virtual Dual inhibition of COX-2 / 5-LOX enzymes based on binding properties of alpha-amyrins, the anti-inflammatory compound as a promising anti-cancer drug

Authors

  • Mohammad Mehdi Ranjbar Razi Vaccine and Sera Institute, Karaj, Iran
  • Vahideh Assadolahi Cellular and Molecular Research Center, Kurdistan University of Medical Sciences, Sanandaj, Iran
  • Mohsen Yazdani Laboratory of Bioinformatics and Drug Design, Pars Silico Bioinformatics Institute, Tehran, Iran
  • Donya Nikaein Academic Center for Education, Culture and Research, Tehran, Iran
  • Behnam Rashidieh Academic Center for Education, Culture and Research, Tehran, Iran

DOI:

https://doi.org/10.17179/excli2016-164

Keywords:

drug discovery, alpha-amyrins, anti cancer drug, Cyclooxygenase-2 (COX2), 5-Lipooxygenase (5-LOX)

Abstract

Hydro-alcoholic fruit extract of Cordia myxa was considerably effective on curing acute inflammation in mouse model. Previous studies suggested significant anti-inflammatory activities as well as potential anticancer agent of α-amyrins in seeds. Inhibition of Cyclooxygenase-2 (COX-2) and 5-Lipooxygenase (5-LOX) is significant in cancer prevention and therapeutics although this inhibition with chemo-drugs has its own side-effects. It is shown that these enzymes pathways are related to several cancers including colon, breast and lung cancer. This study was conducted based on Cordia species' α-amyrins as a safer natural anti-cancer compound for inhibition of COX-2 and 5-LOX enzymes by molecular docking. The X-ray crystal structure of COX2 / 5-LOX enzymes and α-amyrins was retrieved and energetically minimized respectively. The binding site and surface of enzymes were detected. Docking studies were performed by AutoDock 4.2 using Lamarckian genetic algorithm (LGA). Finally drug likeness, molecular pharmacokinetic properties and toxicity of α-amyrins was calculated. Molecular Docking revealed hydrogen and hydrophobic interactions between α-amyrins with both active sites of COX-2 and 5-LOX enzymes. Interestingly, it covalently bonded to Fe cofactor of 5-LOX enzyme and chelated this molecule. Base on binding energies (∆G) α-amyrin has more inhibitory effects on 5-LOX (-10.45 Kcal/mol) than COX-2 (-8.02 Kcal/mol). Analysis of molecular pharmacokinetic parameters suggested that α-amyrins complied with most sets of Lipinski's rules, and so it could be a suitable ligand for docking studies. Eventually, bioactivity score showed α-amyrins possess considerable biological activities as nuclear receptor, enzyme inhibitor, GPCR and protease inhibitor ligand. These results clearly demonstrate that α-amyrins could act as potential highly selective COX-/5-LOX inhibitor. Also, it is a safe compound in comparison with classical non-steroidal anti-inflammatory drugs (NSAIDs) that are known as cancer preventive agents, since it is free of side effects on human body and it can be a promising drug for cancer therapeutics.

Published

2016-03-23

How to Cite

Ranjbar, M. M., Assadolahi, V., Yazdani, M., Nikaein, D., & Rashidieh, B. (2016). Virtual Dual inhibition of COX-2 / 5-LOX enzymes based on binding properties of alpha-amyrins, the anti-inflammatory compound as a promising anti-cancer drug . EXCLI Journal, 15, 238–245. https://doi.org/10.17179/excli2016-164

Issue

Section

Original articles