Competition Between Phenothiazines and BH3 Peptide for the Binding Site of the Antiapoptotic BCL-2 Protein

Competition Between Phenothiazines and BH3 Peptide for the Binding Site of the Antiapoptotic BCL-2 Protein

The study of proteins and mechanisms involved in the apoptosis and new knowledge about cancer's biology are essential for planning new drugs. Tumor cells develop several strategies to gain proliferative advantages, including molecular alterations to evade from apoptosis. Failures in apoptosis c...

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Main Authors: Aline Lagoeiro do Carmo, Fernanda Bettanin, Michell Oliveira Almeida, Simone Queiroz Pantaleão, Tiago Rodrigues, Paula Homem-de-Mello, Kathia Maria Honorio
Format: Article
Language:English
Published: Frontiers Media S.A. 2020-04-01
Series:Frontiers in Chemistry
Subjects:
apoptosis
cancer
BCL-2
BH3
phenothiazines
docking
Online Access:https://www.frontiersin.org/article/10.3389/fchem.2020.00235/full
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spelling doaj-40d6212648a04a8dbe7c14618501d7ac2020-11-25T02:58:20ZengFrontiers Media S.A.Frontiers in Chemistry2296-26462020-04-01810.3389/fchem.2020.00235500971Competition Between Phenothiazines and BH3 Peptide for the Binding Site of the Antiapoptotic BCL-2 ProteinAline Lagoeiro do Carmo0Fernanda Bettanin1Michell Oliveira Almeida2Simone Queiroz Pantaleão3Tiago Rodrigues4Paula Homem-de-Mello5Kathia Maria Honorio6Kathia Maria Honorio7Centro de Ciências Naturais e Humanas, Universidade Federal do ABC, Santo André, BrazilEscola de Artes, Ciências e Humanidades, Universidade de São Paulo (USP), São Paulo, BrazilInstituto de Química de São Carlos, Universidade de São Paulo (USP), São Paulo, BrazilCentro de Ciências Naturais e Humanas, Universidade Federal do ABC, Santo André, BrazilCentro de Ciências Naturais e Humanas, Universidade Federal do ABC, Santo André, BrazilCentro de Ciências Naturais e Humanas, Universidade Federal do ABC, Santo André, BrazilCentro de Ciências Naturais e Humanas, Universidade Federal do ABC, Santo André, BrazilEscola de Artes, Ciências e Humanidades, Universidade de São Paulo (USP), São Paulo, BrazilThe study of proteins and mechanisms involved in the apoptosis and new knowledge about cancer's biology are essential for planning new drugs. Tumor cells develop several strategies to gain proliferative advantages, including molecular alterations to evade from apoptosis. Failures in apoptosis could contribute to cancer pathogenesis, since these defects can cause the accumulation of dividing cells and do not remove genetic variants that have malignant potential. The apoptosis mechanism is composed by proteins that are members of BCL-2 and cysteine-protease families. BH3-only peptides are the “natural” intracellular ligands of BCL-2 family proteins. On the other hand, studies have proved that phenothiazine compounds influence the induction of cellular death. To understand the characteristics of phenothiazines and their effects on tumoral cells and organelles involved in the apoptosis, as well as evaluating their pharmacologic potential, we have carried out computational simulation with the purpose of relating the structures of the phenothiazines with their biological activity. Since the tridimensional (3D) structure of the target protein is known, we have employed the molecular docking approach to study the interactions between compounds and the protein's active site. Hereafter, the molecular dynamics technique was used to verify the temporal evolution of the BCL-2 complexes with phenothiazinic compounds and the BH3 peptide, the stability and the mobility of these molecules in the BCL-2 binding site. From these results, the calculation of binding free energy between the compounds and the biological target was carried out. Thus, it was possible to verify that thioridazine and trifluoperazine tend to increase the stability of the BCL-2 protein and can compete for the binding site with the BH3 peptide.https://www.frontiersin.org/article/10.3389/fchem.2020.00235/fullapoptosiscancerBCL-2BH3phenothiazinesdocking
collection DOAJ
language English
format Article
sources DOAJ
author Aline Lagoeiro do Carmo
Fernanda Bettanin
Michell Oliveira Almeida
Simone Queiroz Pantaleão
Tiago Rodrigues
Paula Homem-de-Mello
Kathia Maria Honorio
Kathia Maria Honorio
spellingShingle Aline Lagoeiro do Carmo
Fernanda Bettanin
Michell Oliveira Almeida
Simone Queiroz Pantaleão
Tiago Rodrigues
Paula Homem-de-Mello
Kathia Maria Honorio
Kathia Maria Honorio
Competition Between Phenothiazines and BH3 Peptide for the Binding Site of the Antiapoptotic BCL-2 Protein
Frontiers in Chemistry
apoptosis
cancer
BCL-2
BH3
phenothiazines
docking
author_facet Aline Lagoeiro do Carmo
Fernanda Bettanin
Michell Oliveira Almeida
Simone Queiroz Pantaleão
Tiago Rodrigues
Paula Homem-de-Mello
Kathia Maria Honorio
Kathia Maria Honorio
author_sort Aline Lagoeiro do Carmo
title Competition Between Phenothiazines and BH3 Peptide for the Binding Site of the Antiapoptotic BCL-2 Protein
title_short Competition Between Phenothiazines and BH3 Peptide for the Binding Site of the Antiapoptotic BCL-2 Protein
title_full Competition Between Phenothiazines and BH3 Peptide for the Binding Site of the Antiapoptotic BCL-2 Protein
title_fullStr Competition Between Phenothiazines and BH3 Peptide for the Binding Site of the Antiapoptotic BCL-2 Protein
title_full_unstemmed Competition Between Phenothiazines and BH3 Peptide for the Binding Site of the Antiapoptotic BCL-2 Protein
title_sort competition between phenothiazines and bh3 peptide for the binding site of the antiapoptotic bcl-2 protein
publisher Frontiers Media S.A.
series Frontiers in Chemistry
issn 2296-2646
publishDate 2020-04-01
description The study of proteins and mechanisms involved in the apoptosis and new knowledge about cancer's biology are essential for planning new drugs. Tumor cells develop several strategies to gain proliferative advantages, including molecular alterations to evade from apoptosis. Failures in apoptosis could contribute to cancer pathogenesis, since these defects can cause the accumulation of dividing cells and do not remove genetic variants that have malignant potential. The apoptosis mechanism is composed by proteins that are members of BCL-2 and cysteine-protease families. BH3-only peptides are the “natural” intracellular ligands of BCL-2 family proteins. On the other hand, studies have proved that phenothiazine compounds influence the induction of cellular death. To understand the characteristics of phenothiazines and their effects on tumoral cells and organelles involved in the apoptosis, as well as evaluating their pharmacologic potential, we have carried out computational simulation with the purpose of relating the structures of the phenothiazines with their biological activity. Since the tridimensional (3D) structure of the target protein is known, we have employed the molecular docking approach to study the interactions between compounds and the protein's active site. Hereafter, the molecular dynamics technique was used to verify the temporal evolution of the BCL-2 complexes with phenothiazinic compounds and the BH3 peptide, the stability and the mobility of these molecules in the BCL-2 binding site. From these results, the calculation of binding free energy between the compounds and the biological target was carried out. Thus, it was possible to verify that thioridazine and trifluoperazine tend to increase the stability of the BCL-2 protein and can compete for the binding site with the BH3 peptide.
topic apoptosis
cancer
BCL-2
BH3
phenothiazines
docking
url https://www.frontiersin.org/article/10.3389/fchem.2020.00235/full
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