Molecular Interaction of Angiotensin-I Converting Enzyme (ACE) with Peptides Derived from Collagen Type i as Analogue for Tilapia By-Product Protein Precursor

Author:

Abd Wahab Nur Suraya1,Anak Yaji Emmy Liza1,Abd Talib Norfahana1,Sabri Mohamad Zulkeflee1,Yong Kelly Tau Len1,Razali Nadia1,Pa'ee Khairul Faizal1

Affiliation:

1. Universiti Kuala Lumpur, Branch Campus Malaysian Institute of Chemical and Engineering Technology

Abstract

The study aimed to investigate the molecular interaction of ACE-inhibitory peptides derived from collagen type I. Collagen type I alpha 1 and alpha 2 were used in this work was to analogue the tilapia by-product protein precursor for ACE-inhibitory peptides production. In silico production of ACE-inhibitory peptides derived collagen type I from BIOPEP was used to simulate peptide-ACE interaction using Autodock Vina. Most potent ACE-inhibitory tri-and di-peptides, Gly-Leu-Pro (GLP IC50 1.62 μM) and Cys-Phe (CF IC50 1.96 μM) derived alpha 1 and Leu-Gly-Pro (LGP IC50 0.72 μM), and Glu-Tyr (EY IC50 2.68 μM) derived alpha 2 were chosen from BIOPEP database. The hydrophobicity of the amino acids is suggested to contribute to bioactivity. These peptides inhibited the active sites of ACE at the C terminal residue. The zinc (II) interacted with all four peptides directly and indirectly. GLP and CY of alpha 1 could share a bond with His 383, His 387, and Glu 411 instead of directly binding to the zinc (II) atom. ACE has a zinc ion in its coordinates with His 383, His 387, and Glu 411. Alpha 2's LGP and EY were directly bound to Zinc (ii) atoms.

Publisher

Trans Tech Publications, Ltd.

Subject

Mechanical Engineering,Mechanics of Materials,Condensed Matter Physics,General Materials Science

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