TRIAGEM VIRTUAL DE COMPOSTOS ANÁLOGOS A FÁRMACOS INIBIDORES DE RECAPTAÇÃO DE SEROTONINA COMO POSSÍVEIS ANTICOLINESTERÁSICOS

Detalhes bibliográficos
Autor(a) principal: Duarte Silveira Grassi Silveira, Antonia
Data de Publicação: 2023
Idioma: por
Título da fonte: Manancial - Repositório Digital da UFSM
dARK ID: ark:/26339/0013000005b99
Texto Completo: http://repositorio.ufsm.br/handle/1/28008
Resumo: Clinically, Alzheimer's disease (AD) is associated with functional and behavioral symptoms, in addition to several cognitive symptoms, which can be explained by the cholinergic neurotransmission deficit. Galantamine, an acetylcholinesterase (AChE) inhibitor compound, has been widely used as the main treatment for AD. Clinical evidence and imaging studies suggest that patients treated with the anticholinesterase inhibitor galantamine in conjunction with antidepressants in the Selective Serotonin Reuptake Inhibitor (SSRI) class may experience additional benefit. Major Depressive Disorder (MDD) currently affects over 350 million people globally. Newer drugs for treating this disorder were approved for use in the late 2000s, among which are the SSRIs. Considering the possible use of SSRIs as anticholinesterases, the present study aims to evaluate the inhibitory character of molecules of natural origin, with chemical structures similar to those from the antidepressants fluoxetine, sertraline, escitalopram and vortioxetine, against the AChE enzyme. A virtual screening was performed based on the substructures of the mentioned antidepressants, in the PubChem, Natural Products Atlas and Drug Bank databases. The compounds that complied with Lipinski's Rule of Five, showed no toxicity and demonstrated a satisfactory LD50 value, underwent the molecular docking protocol. The data obtained revealed the presence of four possible inhibitors: (2'S,11bR)-variecolortin B, (1aR,1bS,6aR,7aR,7bS,11aS)-spiroxin E, (2'R,5'Z,11bR)-variecolortin B and (1aR,1bS,6aS,7aR,7bS,11aS)-spiroxin B. All intermolecular interactions evaluated occurred between compounds and residues, such as Trp-286, Phe-297 and Ser-293, already proven in the literature as present in the active site of the AChE enzyme. However, they showed a slightly lower binding affinity to the enzyme site than the reference inhibitor. All compounds exhibited physicochemical properties favorable to oral bioavailability. These are potential agents for planning and developing new drugs and/or treatments for AD. As this is an in silico study, it is advisable to evaluate it in in vitro tests and, subsequently, in vivo, to determine its real effectiveness.
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spelling TRIAGEM VIRTUAL DE COMPOSTOS ANÁLOGOS A FÁRMACOS INIBIDORES DE RECAPTAÇÃO DE SEROTONINA COMO POSSÍVEIS ANTICOLINESTERÁSICOSDoença de Alzheimer.AcetilcolinesteraseInibidores Seletivos da Recaptação de SerotoninaTriagem VirtualDocking MolecularCNPQ::CIENCIAS EXATAS E DA TERRA::QUIMICAClinically, Alzheimer's disease (AD) is associated with functional and behavioral symptoms, in addition to several cognitive symptoms, which can be explained by the cholinergic neurotransmission deficit. Galantamine, an acetylcholinesterase (AChE) inhibitor compound, has been widely used as the main treatment for AD. Clinical evidence and imaging studies suggest that patients treated with the anticholinesterase inhibitor galantamine in conjunction with antidepressants in the Selective Serotonin Reuptake Inhibitor (SSRI) class may experience additional benefit. Major Depressive Disorder (MDD) currently affects over 350 million people globally. Newer drugs for treating this disorder were approved for use in the late 2000s, among which are the SSRIs. Considering the possible use of SSRIs as anticholinesterases, the present study aims to evaluate the inhibitory character of molecules of natural origin, with chemical structures similar to those from the antidepressants fluoxetine, sertraline, escitalopram and vortioxetine, against the AChE enzyme. A virtual screening was performed based on the substructures of the mentioned antidepressants, in the PubChem, Natural Products Atlas and Drug Bank databases. The compounds that complied with Lipinski's Rule of Five, showed no toxicity and demonstrated a satisfactory LD50 value, underwent the molecular docking protocol. The data obtained revealed the presence of four possible inhibitors: (2'S,11bR)-variecolortin B, (1aR,1bS,6aR,7aR,7bS,11aS)-spiroxin E, (2'R,5'Z,11bR)-variecolortin B and (1aR,1bS,6aS,7aR,7bS,11aS)-spiroxin B. All intermolecular interactions evaluated occurred between compounds and residues, such as Trp-286, Phe-297 and Ser-293, already proven in the literature as present in the active site of the AChE enzyme. However, they showed a slightly lower binding affinity to the enzyme site than the reference inhibitor. All compounds exhibited physicochemical properties favorable to oral bioavailability. These are potential agents for planning and developing new drugs and/or treatments for AD. As this is an in silico study, it is advisable to evaluate it in in vitro tests and, subsequently, in vivo, to determine its real effectiveness.Clinicamente, a Doença de Alzheimer (DA) está associada a sintomas funcionais e comportamentais, além de diversos sintomas cognitivos, que podem ser explicados pelo déficit de neurotransmissão colinérgica. A galantamina, um composto inibidor da enzima acetilcolinesterase (AChE), tem sido amplamente utilizada como principal tratamento contra a DA. Evidências clínicas e estudos de imagens sugerem que pacientes tratados com o inibidor anticolinesterásico galantamina em conjunto com antidepressivos da classe dos Inibidores Seletivos da Recaptação de Serotonina (ISRSs) podem ter benefícios adicionais. O Transtorno Depressivo Maior (TDM) atualmente afeta mais de 350 milhões de pessoas globalmente. Medicamentos mais recentes para tratamento deste transtorno foram aprovados para uso no final da década de 2000, dentre os quais estão os ISRSs. Considerando o possível uso de ISRSs como anticolinesterásicos, o presente estudo tem como objetivo avaliar o caráter inibitório de moléculas de origem natural, com estruturas químicas análogas aos antidepressivos fluoxetina, sertralina, escitalopram e vortioxetina, frente à enzima AChE. Foi realizada uma triagem virtual baseada nas subestruturas dos antidepressivos mencionados, nos bancos de dados PubChem, Natural Products Atlas e Drug Bank. Os compostos que se adequaram à Regra dos Cinco de Lipinski, não apresentaram toxicidade e demonstraram um valor de DL50 satisfatório passaram pelo protocolo de docking molecular. Os dados obtidos revelaram a presença de quatro possíveis inibidores: (2’S,11bR)-variecolortin B, (1aR,1bS,6aR,7aR,7bS,11aS)-spiroxin E, (2’R,5’Z,11bR)-variecolortin B e (1aR,1bS,6aS,7aR,7bS,11aS)-spiroxin B. Todas as interações intermoleculares avaliadas ocorreram entre os compostos e resíduos, tais como Trp-286, Phe-297 e Ser-293, já comprovados na literatura como presentes no sítio ativo da enzima AChE. No entanto, apresentaram uma afinidade de ligação ao sítio da enzima levemente inferior à do inibidor de referência. Todos os compostos exibiram propriedades físicoquímicas favoráveis à biodisponibilidade oral. Estes são potenciais agentes para o planejamento e desenvolvimento de novos medicamentos e/ou tratamentos para DA. Por se tratar de um estudo in silico, aconselha-se sua avaliação em testes in vitro e, posteriormente, in vivo, para determinar sua real eficácia.Universidade Federal de Santa MariaBrasilUFSMCentro de Ciências Naturais e ExatasBatista Teixeira da Rocha, JoãoDuarte Silveira Grassi Silveira, Antonia2023-03-02T11:44:07Z2023-03-02T11:44:07Z2023-02-062023-02-13Trabalho de Conclusão de Curso de Especializaçãoinfo:eu-repo/semantics/publishedVersionapplication/pdfapplication/pdfhttp://repositorio.ufsm.br/handle/1/28008ark:/26339/0013000005b99porinfo:eu-repo/semantics/openAccessreponame:Manancial - Repositório Digital da UFSMinstname:Universidade Federal de Santa Maria (UFSM)instacron:UFSM2023-03-02T11:44:07Zoai:repositorio.ufsm.br:1/28008Biblioteca Digital de Teses e Dissertaçõeshttps://repositorio.ufsm.br/ONGhttps://repositorio.ufsm.br/oai/requestatendimento.sib@ufsm.br||tedebc@gmail.comopendoar:2023-03-02T11:44:07Manancial - Repositório Digital da UFSM - Universidade Federal de Santa Maria (UFSM)false
dc.title.none.fl_str_mv TRIAGEM VIRTUAL DE COMPOSTOS ANÁLOGOS A FÁRMACOS INIBIDORES DE RECAPTAÇÃO DE SEROTONINA COMO POSSÍVEIS ANTICOLINESTERÁSICOS
title TRIAGEM VIRTUAL DE COMPOSTOS ANÁLOGOS A FÁRMACOS INIBIDORES DE RECAPTAÇÃO DE SEROTONINA COMO POSSÍVEIS ANTICOLINESTERÁSICOS
spellingShingle TRIAGEM VIRTUAL DE COMPOSTOS ANÁLOGOS A FÁRMACOS INIBIDORES DE RECAPTAÇÃO DE SEROTONINA COMO POSSÍVEIS ANTICOLINESTERÁSICOS
Duarte Silveira Grassi Silveira, Antonia
Doença de Alzheimer.
Acetilcolinesterase
Inibidores Seletivos da Recaptação de Serotonina
Triagem Virtual
Docking Molecular
CNPQ::CIENCIAS EXATAS E DA TERRA::QUIMICA
title_short TRIAGEM VIRTUAL DE COMPOSTOS ANÁLOGOS A FÁRMACOS INIBIDORES DE RECAPTAÇÃO DE SEROTONINA COMO POSSÍVEIS ANTICOLINESTERÁSICOS
title_full TRIAGEM VIRTUAL DE COMPOSTOS ANÁLOGOS A FÁRMACOS INIBIDORES DE RECAPTAÇÃO DE SEROTONINA COMO POSSÍVEIS ANTICOLINESTERÁSICOS
title_fullStr TRIAGEM VIRTUAL DE COMPOSTOS ANÁLOGOS A FÁRMACOS INIBIDORES DE RECAPTAÇÃO DE SEROTONINA COMO POSSÍVEIS ANTICOLINESTERÁSICOS
title_full_unstemmed TRIAGEM VIRTUAL DE COMPOSTOS ANÁLOGOS A FÁRMACOS INIBIDORES DE RECAPTAÇÃO DE SEROTONINA COMO POSSÍVEIS ANTICOLINESTERÁSICOS
title_sort TRIAGEM VIRTUAL DE COMPOSTOS ANÁLOGOS A FÁRMACOS INIBIDORES DE RECAPTAÇÃO DE SEROTONINA COMO POSSÍVEIS ANTICOLINESTERÁSICOS
author Duarte Silveira Grassi Silveira, Antonia
author_facet Duarte Silveira Grassi Silveira, Antonia
author_role author
dc.contributor.none.fl_str_mv Batista Teixeira da Rocha, João
dc.contributor.author.fl_str_mv Duarte Silveira Grassi Silveira, Antonia
dc.subject.por.fl_str_mv Doença de Alzheimer.
Acetilcolinesterase
Inibidores Seletivos da Recaptação de Serotonina
Triagem Virtual
Docking Molecular
CNPQ::CIENCIAS EXATAS E DA TERRA::QUIMICA
topic Doença de Alzheimer.
Acetilcolinesterase
Inibidores Seletivos da Recaptação de Serotonina
Triagem Virtual
Docking Molecular
CNPQ::CIENCIAS EXATAS E DA TERRA::QUIMICA
description Clinically, Alzheimer's disease (AD) is associated with functional and behavioral symptoms, in addition to several cognitive symptoms, which can be explained by the cholinergic neurotransmission deficit. Galantamine, an acetylcholinesterase (AChE) inhibitor compound, has been widely used as the main treatment for AD. Clinical evidence and imaging studies suggest that patients treated with the anticholinesterase inhibitor galantamine in conjunction with antidepressants in the Selective Serotonin Reuptake Inhibitor (SSRI) class may experience additional benefit. Major Depressive Disorder (MDD) currently affects over 350 million people globally. Newer drugs for treating this disorder were approved for use in the late 2000s, among which are the SSRIs. Considering the possible use of SSRIs as anticholinesterases, the present study aims to evaluate the inhibitory character of molecules of natural origin, with chemical structures similar to those from the antidepressants fluoxetine, sertraline, escitalopram and vortioxetine, against the AChE enzyme. A virtual screening was performed based on the substructures of the mentioned antidepressants, in the PubChem, Natural Products Atlas and Drug Bank databases. The compounds that complied with Lipinski's Rule of Five, showed no toxicity and demonstrated a satisfactory LD50 value, underwent the molecular docking protocol. The data obtained revealed the presence of four possible inhibitors: (2'S,11bR)-variecolortin B, (1aR,1bS,6aR,7aR,7bS,11aS)-spiroxin E, (2'R,5'Z,11bR)-variecolortin B and (1aR,1bS,6aS,7aR,7bS,11aS)-spiroxin B. All intermolecular interactions evaluated occurred between compounds and residues, such as Trp-286, Phe-297 and Ser-293, already proven in the literature as present in the active site of the AChE enzyme. However, they showed a slightly lower binding affinity to the enzyme site than the reference inhibitor. All compounds exhibited physicochemical properties favorable to oral bioavailability. These are potential agents for planning and developing new drugs and/or treatments for AD. As this is an in silico study, it is advisable to evaluate it in in vitro tests and, subsequently, in vivo, to determine its real effectiveness.
publishDate 2023
dc.date.none.fl_str_mv 2023-03-02T11:44:07Z
2023-03-02T11:44:07Z
2023-02-06
2023-02-13
dc.type.driver.fl_str_mv Trabalho de Conclusão de Curso de Especialização
dc.type.status.fl_str_mv info:eu-repo/semantics/publishedVersion
status_str publishedVersion
dc.identifier.uri.fl_str_mv http://repositorio.ufsm.br/handle/1/28008
dc.identifier.dark.fl_str_mv ark:/26339/0013000005b99
url http://repositorio.ufsm.br/handle/1/28008
identifier_str_mv ark:/26339/0013000005b99
dc.language.iso.fl_str_mv por
language por
dc.rights.driver.fl_str_mv info:eu-repo/semantics/openAccess
eu_rights_str_mv openAccess
dc.format.none.fl_str_mv application/pdf
application/pdf
dc.publisher.none.fl_str_mv Universidade Federal de Santa Maria
Brasil
UFSM
Centro de Ciências Naturais e Exatas
publisher.none.fl_str_mv Universidade Federal de Santa Maria
Brasil
UFSM
Centro de Ciências Naturais e Exatas
dc.source.none.fl_str_mv reponame:Manancial - Repositório Digital da UFSM
instname:Universidade Federal de Santa Maria (UFSM)
instacron:UFSM
instname_str Universidade Federal de Santa Maria (UFSM)
instacron_str UFSM
institution UFSM
reponame_str Manancial - Repositório Digital da UFSM
collection Manancial - Repositório Digital da UFSM
repository.name.fl_str_mv Manancial - Repositório Digital da UFSM - Universidade Federal de Santa Maria (UFSM)
repository.mail.fl_str_mv atendimento.sib@ufsm.br||tedebc@gmail.com
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