Investigation of the Flexibility of Protein Kinases Implicated in the Pathology of Alzheimer’s Disease

Investigation of the Flexibility of Protein Kinases Implicated in the Pathology of Alzheimer’s Disease

The pathological characteristics of Alzheimer’s Disease (AD) have been linked to the activity of three particular kinases—Glycogen Synthase Kinase 3β (GSK3β), Cyclin-Dependent Kinase 5 (CDK5) and Extracellular-signal Regulated Kinase 2 (ERK2). As a consequence, the design of selective, potent and d...

Full description

Bibliographic Details
Main Authors: Michael P. Mazanetz, Charles A. Laughton, Peter M. Fischer
Format: Article
Language:English
Published: MDPI AG 2014-06-01
Series:Molecules
Subjects:
active site pressurisation
kinase
structure-based drug design
protein flexibility
molecular dynamics
Online Access:http://www.mdpi.com/1420-3049/19/7/9134
id doaj-1be59b85940c4202a0e070ee093aa5cf
record_format Article
spelling doaj-1be59b85940c4202a0e070ee093aa5cf2020-11-24T23:41:00ZengMDPI AGMolecules1420-30492014-06-011979134915910.3390/molecules19079134molecules19079134Investigation of the Flexibility of Protein Kinases Implicated in the Pathology of Alzheimer’s DiseaseMichael P. Mazanetz0Charles A. Laughton1Peter M. Fischer2Centre for Biomolecular Sciences and School of Pharmacy, University of Nottingham, University Park, Nottingham NG7 2RD, UKCentre for Biomolecular Sciences and School of Pharmacy, University of Nottingham, University Park, Nottingham NG7 2RD, UKCentre for Biomolecular Sciences and School of Pharmacy, University of Nottingham, University Park, Nottingham NG7 2RD, UKThe pathological characteristics of Alzheimer’s Disease (AD) have been linked to the activity of three particular kinases—Glycogen Synthase Kinase 3β (GSK3β), Cyclin-Dependent Kinase 5 (CDK5) and Extracellular-signal Regulated Kinase 2 (ERK2). As a consequence, the design of selective, potent and drug-like inhibitors of these kinases is of particular interest. Structure-based design methods are well-established in the development of kinase inhibitors. However, progress in this field is limited by the difficulty in obtaining X-ray crystal structures suitable for drug design and by the inability of this method to resolve highly flexible regions of the protein that are crucial for ligand binding. To address this issue, we have undertaken a study of human protein kinases CDK5/p25, CDK5, ERK2 and GSK3β using both conventional molecular dynamics (MD) and the new Active Site Pressurisation (ASP) methodology, to look for kinase-specific patterns of flexibility that could be leveraged for the design of selective inhibitors. ASP was used to examine the intrinsic flexibility of the ATP-binding pocket for CDK5/p25, CDK5 and GSK3β where it is shown to be capable of inducing significant conformational changes when compared with X-ray crystal structures. The results from these experiments were used to quantify the dynamics of each protein, which supported the observations made from the conventional MD simulations. Additional information was also derived from the ASP simulations, including the shape of the ATP-binding site and the rigidity of the ATP-binding pocket. These observations may be exploited in the design of selective inhibitors of GSK3β, CDK5 and ERK2.http://www.mdpi.com/1420-3049/19/7/9134active site pressurisationkinasestructure-based drug designprotein flexibilitymolecular dynamics
collection DOAJ
language English
format Article
sources DOAJ
author Michael P. Mazanetz
Charles A. Laughton
Peter M. Fischer
spellingShingle Michael P. Mazanetz
Charles A. Laughton
Peter M. Fischer
Investigation of the Flexibility of Protein Kinases Implicated in the Pathology of Alzheimer’s Disease
Molecules
active site pressurisation
kinase
structure-based drug design
protein flexibility
molecular dynamics
author_facet Michael P. Mazanetz
Charles A. Laughton
Peter M. Fischer
author_sort Michael P. Mazanetz
title Investigation of the Flexibility of Protein Kinases Implicated in the Pathology of Alzheimer’s Disease
title_short Investigation of the Flexibility of Protein Kinases Implicated in the Pathology of Alzheimer’s Disease
title_full Investigation of the Flexibility of Protein Kinases Implicated in the Pathology of Alzheimer’s Disease
title_fullStr Investigation of the Flexibility of Protein Kinases Implicated in the Pathology of Alzheimer’s Disease
title_full_unstemmed Investigation of the Flexibility of Protein Kinases Implicated in the Pathology of Alzheimer’s Disease
title_sort investigation of the flexibility of protein kinases implicated in the pathology of alzheimer’s disease
publisher MDPI AG
series Molecules
issn 1420-3049
publishDate 2014-06-01
description The pathological characteristics of Alzheimer’s Disease (AD) have been linked to the activity of three particular kinases—Glycogen Synthase Kinase 3β (GSK3β), Cyclin-Dependent Kinase 5 (CDK5) and Extracellular-signal Regulated Kinase 2 (ERK2). As a consequence, the design of selective, potent and drug-like inhibitors of these kinases is of particular interest. Structure-based design methods are well-established in the development of kinase inhibitors. However, progress in this field is limited by the difficulty in obtaining X-ray crystal structures suitable for drug design and by the inability of this method to resolve highly flexible regions of the protein that are crucial for ligand binding. To address this issue, we have undertaken a study of human protein kinases CDK5/p25, CDK5, ERK2 and GSK3β using both conventional molecular dynamics (MD) and the new Active Site Pressurisation (ASP) methodology, to look for kinase-specific patterns of flexibility that could be leveraged for the design of selective inhibitors. ASP was used to examine the intrinsic flexibility of the ATP-binding pocket for CDK5/p25, CDK5 and GSK3β where it is shown to be capable of inducing significant conformational changes when compared with X-ray crystal structures. The results from these experiments were used to quantify the dynamics of each protein, which supported the observations made from the conventional MD simulations. Additional information was also derived from the ASP simulations, including the shape of the ATP-binding site and the rigidity of the ATP-binding pocket. These observations may be exploited in the design of selective inhibitors of GSK3β, CDK5 and ERK2.
topic active site pressurisation
kinase
structure-based drug design
protein flexibility
molecular dynamics
url http://www.mdpi.com/1420-3049/19/7/9134
work_keys_str_mv AT michaelpmazanetz investigationoftheflexibilityofproteinkinasesimplicatedinthepathologyofalzheimersdisease
AT charlesalaughton investigationoftheflexibilityofproteinkinasesimplicatedinthepathologyofalzheimersdisease
AT petermfischer investigationoftheflexibilityofproteinkinasesimplicatedinthepathologyofalzheimersdisease
_version_ 1725508344264785920

Similar Items