Mechanisms of Peptide Hydrolysis by Aspartyl and Metalloproteases

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Date

2016

Journal Title

Journal ISSN

Volume Title

Publisher

Royal Society of Chemistry

Open Access Color

Green Open Access

No

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Abstract

Peptide hydrolysis has been involved in a wide range of biological, biotechnological, and industrial applications. In this perspective, the mechanisms of three distinct peptide bond cleaving enzymes, beta secretase (BACE1), insulin degrading enzyme (IDE), and bovine lens leucine aminopeptidase (BILAP), have been discussed. BACE1 is a catalytic Asp dyad [Asp, Asp(-)] containing aspartyl protease, while IDE and BILAP are mononuclear [Zn(His, His, Glu)] and binuclear [Zn1(Asp, Glu, Asp)-Zn2(Lys, Glu, Asp, Asp)] core possessing metallopeptidases, respectively. Specifically, enzyme-substrate interactions and the roles of metal ion(s), the ligand environment, second coordination shell residues, and the protein environment in the functioning of these enzymes have been elucidated. This information will be useful to design small inhibitors, activators, and synthetic analogues of these enzymes for biomedical, biotechnological, and industrial applications.

Description

Prabhakar, Rajeev/0000-0003-1137-1272; Paul, Thomas/0000-0003-3884-2150; Özbil, Mehmet/0000-0002-1465-7674

Keywords

570, Hydrolysis, 610, Ligands, Insulysin, Protein Structure, Tertiary, Leucyl Aminopeptidase, Zinc, Catalytic Domain, Biocatalysis, Animals, Thermodynamics, Cattle, Amyloid Precursor Protein Secretases, Peptides

Fields of Science

0301 basic medicine, 0303 health sciences, 03 medical and health sciences

Citation

WoS Q

Q2

Scopus Q

Q2
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OpenCitations Citation Count
15

Source

Physical Chemistry Chemical Physics

Volume

18

Issue

36

Start Page

24790

End Page

24801
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Citations

CrossRef : 14

Scopus : 15

PubMed : 2

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Mendeley Readers : 24

Web of Science™ Citations

13

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