The schistosomiasis spleenOME : unveiling the proteomic landscape of splenomegaly using label-free mass spectrometry.

Detalhes bibliográficos
Autor(a) principal: Cosenza Contreras, Miguel de Jesus
Data de Publicação: 2019
Outros Autores: Castro, Renata Alves de Oliveira e, Mattei, Bruno, Campos, Jonatan Marques, Silva, Gustavo Gonçalves, Paiva, Nívia Carolina Nogueira de, Soares, Rodrigo Dian de Oliveira Aguiar, Carneiro, Cláudia Martins, Afonso, Luís Carlos Crocco, Borges, William de Castro
Tipo de documento: Artigo
Idioma: eng
Título da fonte: Repositório Institucional da UFOP
Texto Completo: http://www.repositorio.ufop.br/handle/123456789/10841
Resumo: Schistosomiasis is a neglected parasitic disease that affects millions of people worldwide and is caused by helminth parasites from the genus Schistosoma. When caused by S. mansoni, it is associated with the development of a hepatosplenic disease caused by an intense immune response to the important antigenic contribution of adult worms and to the presence of eggs trapped in liver tissue. Although the importance of the spleen for the establishment of immune pathology is widely accepted, it has received little attention in terms of the molecular mechanisms operating in response to the infection. Here, we interrogated the spleen proteome using a label-free shotgun approach for the potential discovery of molecular mechanisms associated to the peak of the acute phase of inflammation and the development of splenomegaly in the murine model. Over fifteen hundred proteins were identified in both infected and control individuals and 325 of those proteins were differentially expressed. Two hundred and forty-two proteins were found upregulated in infected individuals while 83 were downregulated. Functional enrichment analyses for differentially expressed proteins showed that most of them were categorized within pathways of innate and adaptive immunity, DNA replication, vesicle transport and catabolic metabolism. There was an important contribution of granulocyte proteins and antigen processing and presentation pathways were augmented, with the increased expression of MHC class II molecules but the negative regulation of cysteine and serine proteases. Several proteins related to RNA processing were upregulated, including splicing factors. We also found indications of metabolic reprogramming in spleen cells with downregulation of proteins related to mitochondrial metabolism. Ex-vivo imunophenotyping of spleen cells allowed us to attribute the higher abundance of MHC II detected by mass spectrometry to increased number of macrophages (F4/80+/MHC II+ cells) in the infected condition. We believe these findings add novel insights for the understanding of the immune mechanisms associated with the establishment of schistosomiasis and the processes of immune modulation implied in the host-parasite interactions.
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spelling Cosenza Contreras, Miguel de JesusCastro, Renata Alves de Oliveira eMattei, BrunoCampos, Jonatan MarquesSilva, Gustavo GonçalvesPaiva, Nívia Carolina Nogueira deSoares, Rodrigo Dian de Oliveira AguiarCarneiro, Cláudia MartinsAfonso, Luís Carlos CroccoBorges, William de Castro2019-03-27T17:16:56Z2019-03-27T17:16:56Z2019COSENZA CONTRERAS, M. de J. et al. The schistosomiasis spleenOME : unveiling the proteomic landscape of splenomegaly using label-free mass spectrometry. Frontiers in Immunology, v. 9, p. 1-17, jan. 2019. Disponível em: <https://www.frontiersin.org/articles/10.3389/fimmu.2018.03137/full>. Acesso em: 21 fev. 2019.16634365http://www.repositorio.ufop.br/handle/123456789/10841Schistosomiasis is a neglected parasitic disease that affects millions of people worldwide and is caused by helminth parasites from the genus Schistosoma. When caused by S. mansoni, it is associated with the development of a hepatosplenic disease caused by an intense immune response to the important antigenic contribution of adult worms and to the presence of eggs trapped in liver tissue. Although the importance of the spleen for the establishment of immune pathology is widely accepted, it has received little attention in terms of the molecular mechanisms operating in response to the infection. Here, we interrogated the spleen proteome using a label-free shotgun approach for the potential discovery of molecular mechanisms associated to the peak of the acute phase of inflammation and the development of splenomegaly in the murine model. Over fifteen hundred proteins were identified in both infected and control individuals and 325 of those proteins were differentially expressed. Two hundred and forty-two proteins were found upregulated in infected individuals while 83 were downregulated. Functional enrichment analyses for differentially expressed proteins showed that most of them were categorized within pathways of innate and adaptive immunity, DNA replication, vesicle transport and catabolic metabolism. There was an important contribution of granulocyte proteins and antigen processing and presentation pathways were augmented, with the increased expression of MHC class II molecules but the negative regulation of cysteine and serine proteases. Several proteins related to RNA processing were upregulated, including splicing factors. We also found indications of metabolic reprogramming in spleen cells with downregulation of proteins related to mitochondrial metabolism. Ex-vivo imunophenotyping of spleen cells allowed us to attribute the higher abundance of MHC II detected by mass spectrometry to increased number of macrophages (F4/80+/MHC II+ cells) in the infected condition. We believe these findings add novel insights for the understanding of the immune mechanisms associated with the establishment of schistosomiasis and the processes of immune modulation implied in the host-parasite interactions.This is an open-access article distributed under the terms of the Creative Commons Attribution License (CC BY). The use, distribution or reproduction in other forums is permitted, provided the original author(s) and the copyright owner are credited and that the original publication in this journal is cited, in accordance with accepted academic practice. No use, distribution or reproduction is permitted which does not comply with these terms. Fonte: o próprio artigo.info:eu-repo/semantics/openAccessSchistosoma mansonHost-parasite interactionsProteomeHelminthiasisAcute inflammationThe schistosomiasis spleenOME : unveiling the proteomic landscape of splenomegaly using label-free mass spectrometry.info:eu-repo/semantics/publishedVersioninfo:eu-repo/semantics/articleengreponame:Repositório Institucional da UFOPinstname:Universidade Federal de Ouro Preto (UFOP)instacron:UFOPLICENSElicense.txtlicense.txttext/plain; charset=utf-8924http://www.repositorio.ufop.br/bitstream/123456789/10841/2/license.txt62604f8d955274beb56c80ce1ee5dcaeMD52ORIGINALARTIGO_SchistosomiasisSpleenomeUnveiling.pdfARTIGO_SchistosomiasisSpleenomeUnveiling.pdfapplication/pdf2001971http://www.repositorio.ufop.br/bitstream/123456789/10841/1/ARTIGO_SchistosomiasisSpleenomeUnveiling.pdfe21ebcf5dc9fa63190cf847855887f3eMD51123456789/108412019-03-27 13:16:56.375oai:localhost: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ório InstitucionalPUBhttp://www.repositorio.ufop.br/oai/requestrepositorio@ufop.edu.bropendoar:32332019-03-27T17:16:56Repositório Institucional da UFOP - Universidade Federal de Ouro Preto (UFOP)false
dc.title.pt_BR.fl_str_mv The schistosomiasis spleenOME : unveiling the proteomic landscape of splenomegaly using label-free mass spectrometry.
title The schistosomiasis spleenOME : unveiling the proteomic landscape of splenomegaly using label-free mass spectrometry.
spellingShingle The schistosomiasis spleenOME : unveiling the proteomic landscape of splenomegaly using label-free mass spectrometry.
Cosenza Contreras, Miguel de Jesus
Schistosoma manson
Host-parasite interactions
Proteome
Helminthiasis
Acute inflammation
title_short The schistosomiasis spleenOME : unveiling the proteomic landscape of splenomegaly using label-free mass spectrometry.
title_full The schistosomiasis spleenOME : unveiling the proteomic landscape of splenomegaly using label-free mass spectrometry.
title_fullStr The schistosomiasis spleenOME : unveiling the proteomic landscape of splenomegaly using label-free mass spectrometry.
title_full_unstemmed The schistosomiasis spleenOME : unveiling the proteomic landscape of splenomegaly using label-free mass spectrometry.
title_sort The schistosomiasis spleenOME : unveiling the proteomic landscape of splenomegaly using label-free mass spectrometry.
author Cosenza Contreras, Miguel de Jesus
author_facet Cosenza Contreras, Miguel de Jesus
Castro, Renata Alves de Oliveira e
Mattei, Bruno
Campos, Jonatan Marques
Silva, Gustavo Gonçalves
Paiva, Nívia Carolina Nogueira de
Soares, Rodrigo Dian de Oliveira Aguiar
Carneiro, Cláudia Martins
Afonso, Luís Carlos Crocco
Borges, William de Castro
author_role author
author2 Castro, Renata Alves de Oliveira e
Mattei, Bruno
Campos, Jonatan Marques
Silva, Gustavo Gonçalves
Paiva, Nívia Carolina Nogueira de
Soares, Rodrigo Dian de Oliveira Aguiar
Carneiro, Cláudia Martins
Afonso, Luís Carlos Crocco
Borges, William de Castro
author2_role author
author
author
author
author
author
author
author
author
dc.contributor.author.fl_str_mv Cosenza Contreras, Miguel de Jesus
Castro, Renata Alves de Oliveira e
Mattei, Bruno
Campos, Jonatan Marques
Silva, Gustavo Gonçalves
Paiva, Nívia Carolina Nogueira de
Soares, Rodrigo Dian de Oliveira Aguiar
Carneiro, Cláudia Martins
Afonso, Luís Carlos Crocco
Borges, William de Castro
dc.subject.por.fl_str_mv Schistosoma manson
Host-parasite interactions
Proteome
Helminthiasis
Acute inflammation
topic Schistosoma manson
Host-parasite interactions
Proteome
Helminthiasis
Acute inflammation
description Schistosomiasis is a neglected parasitic disease that affects millions of people worldwide and is caused by helminth parasites from the genus Schistosoma. When caused by S. mansoni, it is associated with the development of a hepatosplenic disease caused by an intense immune response to the important antigenic contribution of adult worms and to the presence of eggs trapped in liver tissue. Although the importance of the spleen for the establishment of immune pathology is widely accepted, it has received little attention in terms of the molecular mechanisms operating in response to the infection. Here, we interrogated the spleen proteome using a label-free shotgun approach for the potential discovery of molecular mechanisms associated to the peak of the acute phase of inflammation and the development of splenomegaly in the murine model. Over fifteen hundred proteins were identified in both infected and control individuals and 325 of those proteins were differentially expressed. Two hundred and forty-two proteins were found upregulated in infected individuals while 83 were downregulated. Functional enrichment analyses for differentially expressed proteins showed that most of them were categorized within pathways of innate and adaptive immunity, DNA replication, vesicle transport and catabolic metabolism. There was an important contribution of granulocyte proteins and antigen processing and presentation pathways were augmented, with the increased expression of MHC class II molecules but the negative regulation of cysteine and serine proteases. Several proteins related to RNA processing were upregulated, including splicing factors. We also found indications of metabolic reprogramming in spleen cells with downregulation of proteins related to mitochondrial metabolism. Ex-vivo imunophenotyping of spleen cells allowed us to attribute the higher abundance of MHC II detected by mass spectrometry to increased number of macrophages (F4/80+/MHC II+ cells) in the infected condition. We believe these findings add novel insights for the understanding of the immune mechanisms associated with the establishment of schistosomiasis and the processes of immune modulation implied in the host-parasite interactions.
publishDate 2019
dc.date.accessioned.fl_str_mv 2019-03-27T17:16:56Z
dc.date.available.fl_str_mv 2019-03-27T17:16:56Z
dc.date.issued.fl_str_mv 2019
dc.type.status.fl_str_mv info:eu-repo/semantics/publishedVersion
dc.type.driver.fl_str_mv info:eu-repo/semantics/article
format article
status_str publishedVersion
dc.identifier.citation.fl_str_mv COSENZA CONTRERAS, M. de J. et al. The schistosomiasis spleenOME : unveiling the proteomic landscape of splenomegaly using label-free mass spectrometry. Frontiers in Immunology, v. 9, p. 1-17, jan. 2019. Disponível em: <https://www.frontiersin.org/articles/10.3389/fimmu.2018.03137/full>. Acesso em: 21 fev. 2019.
dc.identifier.uri.fl_str_mv http://www.repositorio.ufop.br/handle/123456789/10841
dc.identifier.issn.none.fl_str_mv 16634365
identifier_str_mv COSENZA CONTRERAS, M. de J. et al. The schistosomiasis spleenOME : unveiling the proteomic landscape of splenomegaly using label-free mass spectrometry. Frontiers in Immunology, v. 9, p. 1-17, jan. 2019. Disponível em: <https://www.frontiersin.org/articles/10.3389/fimmu.2018.03137/full>. Acesso em: 21 fev. 2019.
16634365
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