NOVEL HIGH AFFINITY INHIBITORS BASEDON THE CHEMICAL MODIFICATIONS OF 3, 4 DIHYDROXY BENZOIC ACID : DOCKING SIMULATIONS ON LIPOXYGENASE

Authors

  • A BENSEGUENI Université Constantine 1
  • A CHIKHI Université Constantine 1
  • M BENCHARIF Université Constantine 1

Keywords:

Binding Energy, Docking, Modeling, Enzyme-Inhibitor Complex, Lipoxygenase, Interaction protein-ligand

Abstract

Modeling enzyme-inhiubitor interactions using FlexX program allowed to design novel high affinity inhibitors of soybean lipoxygenase (LOX-3). Docking results show that the binding energy of the enzyme with its inhibitor 3,4 dihydroxy benzoic acid (DHB) is ∆G = -10.564 Kj/mol. .This binding energy enhances when a hydroxyl group is added on the ring of DHB (∆G = -16.959 Kj /mol) or its carboxylic group is replaced by other functional groups, particularly a methyl hydroxyl group (∆G = - 21.127 Kj/mol). Docking study may be useful to improve the biological activity of a compound for a given target.

Author Biographies

A BENSEGUENI, Université Constantine 1

Department of Biology

A CHIKHI, Université Constantine 1

Department of Biology

M BENCHARIF, Université Constantine 1

Laboratory of Materials Chemistry,

Department of Chemistry, Faculty of Science

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Published

2007-12-01

How to Cite

BENSEGUENI, A., CHIKHI, A., & BENCHARIF, M. (2007). NOVEL HIGH AFFINITY INHIBITORS BASEDON THE CHEMICAL MODIFICATIONS OF 3, 4 DIHYDROXY BENZOIC ACID : DOCKING SIMULATIONS ON LIPOXYGENASE. Sciences & Technology. C, Biotechnologies, (26), 69–73. Retrieved from https://revue.umc.edu.dz/c/article/view/378

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