Benzo[b]thiophene-based bis-ureas as inhibitors of Aβ-LilrB2 aggregates in Alzheimer’s Disease: an in silico investigation
| Autor(a) principal: | |
|---|---|
| Data de Publicação: | 2023 |
| Tipo de documento: | Dissertação |
| Idioma: | eng |
| Título da fonte: | Repositório Científico de Acesso Aberto de Portugal (Repositórios Cientìficos) |
| Texto Completo: | http://hdl.handle.net/10773/39541 |
Resumo: | Alzheimer’s Disease (AD) is a chronic neurodegenerative disease with high socioeconomic costs. Due to its complexity, existing therapies only alleviate symptoms and/or delay its progression. The formation of Amyloid β (Aβ) protein aggregates resulting from the breakdown of Aβ precursor protein (APP) has been identified as one of the factors responsible for the onset and development of AD. The accumulation of Aβ aggregates in the brain leads to neuronal cell death due to the diffusion of oligomers (AβOs). AβOs act through multiple mechanisms by interacting with receptors located on the cell surface. One of these receptors, with high affinity for AβOs, is the Leukocyte Immunoglobulin-Like Receptor B2 (LilrB2), expressed in the cerebral microglia. The association of AβOs with LilrB2 and with the Triggering Receptor Expressed on Myeloid Cells 2 (TREM2) impairs the immune response to the diffusion of Aβ aggregates, leading to loss of synaptic plasticity and the memory deficits that characterize AD. Therefore, the inhibition of LilrB2 by supramolecular association with drug-like molecules emerges as a possible treatment of this pathology. In this context, the present dissertation presents an investigation at the molecular level of the interaction of AβOs with LilrB2 and with two sets of ligands. These studies were carried out using docking methods, followed by molecular dynamics (MD) simulations and free energy calculations using Molecular Mechanics/Generalized Born Surface Area (MM/GBSA). The first set of molecules (A) consists of six drugs with diverse structures and different affinities for LilrB2, as demonstrated in one experimental study reported in the literature. The second set of molecules (B) is composed of ten bis-ureas obtained by coupling ortho-phenylenediamine with two benzo[b]thiophenes through the Cα, Cβ, or Cy carbons of this heterocyclic ring. The B-series comprises structural isomers with different shapes, varied lipophilic character, and different putative affinities for the amino acids in the binding groove of LilrB2, determined by different degrees of fluorination. The α derivatives, with extended structures, show higher affinity for the hydrophobic cavity of LilrB2, even when compared to the molecules in set A, due to hydrogen bonding coupled with hydrophobic interactions with amino acids Asp36, Val38, Val114, and Pro164 of the cavity. This computational study indicated a potential repositioning for the molecules in the B-series, initially designed and developed for transmembrane transport of anions in the context of channel replacement therapies in diseases such as Cystic Fibrosis (CF). |
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Benzo[b]thiophene-based bis-ureas as inhibitors of Aβ-LilrB2 aggregates in Alzheimer’s Disease: an in silico investigationAlzheimer’s DiseaseDrug discoveryAβ Aggregates-LilrB2Benzo[b]thiophenebased Bis-ureasMolecular dynamicsFree energy calculationsAlzheimer’s Disease (AD) is a chronic neurodegenerative disease with high socioeconomic costs. Due to its complexity, existing therapies only alleviate symptoms and/or delay its progression. The formation of Amyloid β (Aβ) protein aggregates resulting from the breakdown of Aβ precursor protein (APP) has been identified as one of the factors responsible for the onset and development of AD. The accumulation of Aβ aggregates in the brain leads to neuronal cell death due to the diffusion of oligomers (AβOs). AβOs act through multiple mechanisms by interacting with receptors located on the cell surface. One of these receptors, with high affinity for AβOs, is the Leukocyte Immunoglobulin-Like Receptor B2 (LilrB2), expressed in the cerebral microglia. The association of AβOs with LilrB2 and with the Triggering Receptor Expressed on Myeloid Cells 2 (TREM2) impairs the immune response to the diffusion of Aβ aggregates, leading to loss of synaptic plasticity and the memory deficits that characterize AD. Therefore, the inhibition of LilrB2 by supramolecular association with drug-like molecules emerges as a possible treatment of this pathology. In this context, the present dissertation presents an investigation at the molecular level of the interaction of AβOs with LilrB2 and with two sets of ligands. These studies were carried out using docking methods, followed by molecular dynamics (MD) simulations and free energy calculations using Molecular Mechanics/Generalized Born Surface Area (MM/GBSA). The first set of molecules (A) consists of six drugs with diverse structures and different affinities for LilrB2, as demonstrated in one experimental study reported in the literature. The second set of molecules (B) is composed of ten bis-ureas obtained by coupling ortho-phenylenediamine with two benzo[b]thiophenes through the Cα, Cβ, or Cy carbons of this heterocyclic ring. The B-series comprises structural isomers with different shapes, varied lipophilic character, and different putative affinities for the amino acids in the binding groove of LilrB2, determined by different degrees of fluorination. The α derivatives, with extended structures, show higher affinity for the hydrophobic cavity of LilrB2, even when compared to the molecules in set A, due to hydrogen bonding coupled with hydrophobic interactions with amino acids Asp36, Val38, Val114, and Pro164 of the cavity. This computational study indicated a potential repositioning for the molecules in the B-series, initially designed and developed for transmembrane transport of anions in the context of channel replacement therapies in diseases such as Cystic Fibrosis (CF).A Doença de Alzheimer (AD) é uma doença neurodegenerativa crónica com elevados custos socioeconómicos. Devido à sua complexidade, as terapêuticas existentes apenas atenuam os sintomas e/ou retardam a sua progressão. A formação de agregados proteicos β Amilóide (Aβ) resultantes da decomposição da proteína precursora Aβ (APP) tem sido identificada como um dos fatores responsáveis pelo aparecimento e desenvolvimento da AD. A acumulação de agregados Aβ no cérebro causa a morte das células neuronais, devido à difusão de oligómeros (AβOs). Os AβOs atuam por meio de vários mecanismos, interagindo com recetores localizados na superfície celular. Um destes recetores, com afinidade elevada para AβOs, é o Recetor B2 de Leucócitos do Tipo Imunoglobulina (LilrB2), expresso na microglia cerebral. A associação de AβOs a LilrB2 e ao Recetor de Desencadeamento Expresso em Células Mielóides 2 (TREM2) prejudica a resposta imunológica à difusão de agregados Aβ, levando à perda da plasticidade sináptica e aos défices de memória que caracterizam a AD. Assim, a inibição de LilrB2 por associação supramolecular com moléculas com potencial farmacológico ("drug-like molecules") surge como uma hipótese possível para o tratamento desta patologia. Neste contexto, na presente dissertação apresenta-se uma investigação ao nível molecular da interação de AβO com LilrB2 e com dois conjuntos de ligandos. Estes estudos foram efetuados por métodos de "docking", seguidos por simulações de dinâmica molecular (MD) e cálculos de energia livre por Mecânica Molecular/Área de Superfície Generalizada de Born (MM/GBSA). O primeiro conjunto de moléculas (A) é constituído por seis fármacos, com estruturas diversas e diferentes afinidades para LilrB2, reportado anteriormente na literatura, num estudo experimental. A segunda série de moléculas (B) é composta por dez bis-ureias obtidas por acoplamento de orto-fenilenodiamina com dois benzo[b]tiofenos através dos carbonos Cα, Cβ, ou Cy deste anel heterocíclico. A série B engloba isómeros estruturais com formas diferentes, com caráter lipofílico variado, e afinidades putativas diferentes para os aminoácidos da cavidade de ligação de LilrB2, dado por diferentes graus de fluorinação. Os derivados α, com estruturas estendidas, apresentam uma afinidade superior para a cavidade hidrofóbica do LilrB2, mesmo quando comparada com as moléculas do conjunto A, devido a ligações de hidrogénio acopladas com interações hidrofóbicas com os aminoácidos Asp36, Val38, Val114 e Pro164 da cavidade. Este estudo computacional indicou uma nova aplicação, através do reposicionamento das moléculas da série B, inicialmente desenhadas e desenvolvidas para o transporte transmembranar de aniões no âmbito de terapias de substituição de canal em doenças como a Fibrose Cística (CF).2025-07-07T00:00:00Z2023-07-03T00:00:00Z2023-07-03info:eu-repo/semantics/publishedVersioninfo:eu-repo/semantics/masterThesisapplication/pdfhttp://hdl.handle.net/10773/39541engSantos, Joel José Pereirainfo:eu-repo/semantics/embargoedAccessreponame:Repositório Científico de Acesso Aberto de Portugal (Repositórios Cientìficos)instname:Agência para a Sociedade do Conhecimento (UMIC) - FCT - Sociedade da Informaçãoinstacron:RCAAP2024-02-22T12:17:15Zoai:ria.ua.pt:10773/39541Portal AgregadorONGhttps://www.rcaap.pt/oai/openaireopendoar:71602024-03-20T03:09:42.557324Repositório Científico de Acesso Aberto de Portugal (Repositórios Cientìficos) - Agência para a Sociedade do Conhecimento (UMIC) - FCT - Sociedade da Informaçãofalse |
| dc.title.none.fl_str_mv |
Benzo[b]thiophene-based bis-ureas as inhibitors of Aβ-LilrB2 aggregates in Alzheimer’s Disease: an in silico investigation |
| title |
Benzo[b]thiophene-based bis-ureas as inhibitors of Aβ-LilrB2 aggregates in Alzheimer’s Disease: an in silico investigation |
| spellingShingle |
Benzo[b]thiophene-based bis-ureas as inhibitors of Aβ-LilrB2 aggregates in Alzheimer’s Disease: an in silico investigation Santos, Joel José Pereira Alzheimer’s Disease Drug discovery Aβ Aggregates-LilrB2 Benzo[b]thiophenebased Bis-ureas Molecular dynamics Free energy calculations |
| title_short |
Benzo[b]thiophene-based bis-ureas as inhibitors of Aβ-LilrB2 aggregates in Alzheimer’s Disease: an in silico investigation |
| title_full |
Benzo[b]thiophene-based bis-ureas as inhibitors of Aβ-LilrB2 aggregates in Alzheimer’s Disease: an in silico investigation |
| title_fullStr |
Benzo[b]thiophene-based bis-ureas as inhibitors of Aβ-LilrB2 aggregates in Alzheimer’s Disease: an in silico investigation |
| title_full_unstemmed |
Benzo[b]thiophene-based bis-ureas as inhibitors of Aβ-LilrB2 aggregates in Alzheimer’s Disease: an in silico investigation |
| title_sort |
Benzo[b]thiophene-based bis-ureas as inhibitors of Aβ-LilrB2 aggregates in Alzheimer’s Disease: an in silico investigation |
| author |
Santos, Joel José Pereira |
| author_facet |
Santos, Joel José Pereira |
| author_role |
author |
| dc.contributor.author.fl_str_mv |
Santos, Joel José Pereira |
| dc.subject.por.fl_str_mv |
Alzheimer’s Disease Drug discovery Aβ Aggregates-LilrB2 Benzo[b]thiophenebased Bis-ureas Molecular dynamics Free energy calculations |
| topic |
Alzheimer’s Disease Drug discovery Aβ Aggregates-LilrB2 Benzo[b]thiophenebased Bis-ureas Molecular dynamics Free energy calculations |
| description |
Alzheimer’s Disease (AD) is a chronic neurodegenerative disease with high socioeconomic costs. Due to its complexity, existing therapies only alleviate symptoms and/or delay its progression. The formation of Amyloid β (Aβ) protein aggregates resulting from the breakdown of Aβ precursor protein (APP) has been identified as one of the factors responsible for the onset and development of AD. The accumulation of Aβ aggregates in the brain leads to neuronal cell death due to the diffusion of oligomers (AβOs). AβOs act through multiple mechanisms by interacting with receptors located on the cell surface. One of these receptors, with high affinity for AβOs, is the Leukocyte Immunoglobulin-Like Receptor B2 (LilrB2), expressed in the cerebral microglia. The association of AβOs with LilrB2 and with the Triggering Receptor Expressed on Myeloid Cells 2 (TREM2) impairs the immune response to the diffusion of Aβ aggregates, leading to loss of synaptic plasticity and the memory deficits that characterize AD. Therefore, the inhibition of LilrB2 by supramolecular association with drug-like molecules emerges as a possible treatment of this pathology. In this context, the present dissertation presents an investigation at the molecular level of the interaction of AβOs with LilrB2 and with two sets of ligands. These studies were carried out using docking methods, followed by molecular dynamics (MD) simulations and free energy calculations using Molecular Mechanics/Generalized Born Surface Area (MM/GBSA). The first set of molecules (A) consists of six drugs with diverse structures and different affinities for LilrB2, as demonstrated in one experimental study reported in the literature. The second set of molecules (B) is composed of ten bis-ureas obtained by coupling ortho-phenylenediamine with two benzo[b]thiophenes through the Cα, Cβ, or Cy carbons of this heterocyclic ring. The B-series comprises structural isomers with different shapes, varied lipophilic character, and different putative affinities for the amino acids in the binding groove of LilrB2, determined by different degrees of fluorination. The α derivatives, with extended structures, show higher affinity for the hydrophobic cavity of LilrB2, even when compared to the molecules in set A, due to hydrogen bonding coupled with hydrophobic interactions with amino acids Asp36, Val38, Val114, and Pro164 of the cavity. This computational study indicated a potential repositioning for the molecules in the B-series, initially designed and developed for transmembrane transport of anions in the context of channel replacement therapies in diseases such as Cystic Fibrosis (CF). |
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2023 |
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2023-07-03T00:00:00Z 2023-07-03 2025-07-07T00:00:00Z |
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info:eu-repo/semantics/publishedVersion |
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