The kallikrein-kinin system in experimental Chagas disease: a paradigm to investigate the impact of inflammatory edema on GPCR-mediated pathways of host cell invasion by Trypanosoma cruzi

Chronic chagasic myocarditis (CCM) depends on Trypanosoma cruzi persistence in the myocardium. Studies of the proteolytic mechanisms governing host/parasite balance in peripheral sites of T. cruzi infection revealed that tissue culture trypomastigotes (TCTs) elicit inflammatory edema and stimulate p...

Descripción completa

Detalles Bibliográficos
Autores principales: Scharfstein, Julio, Andrade, Daniele, Svensjö, Erik, Oliveira, Ana Carolina, Nascimento, Clarissa R.
Formato: Online Artículo Texto
Lenguaje:English
Publicado: Frontiers Media S.A. 2013
Materias:
Immunology
Acceso en línea:https://www.ncbi.nlm.nih.gov/pmc/articles/PMC3555122/
https://www.ncbi.nlm.nih.gov/pubmed/23355836
http://dx.doi.org/10.3389/fimmu.2012.00396
_version_ 1782257005760610304
author Scharfstein, Julio
Andrade, Daniele
Svensjö, Erik
Oliveira, Ana Carolina
Nascimento, Clarissa R.
author_facet Scharfstein, Julio
Andrade, Daniele
Svensjö, Erik
Oliveira, Ana Carolina
Nascimento, Clarissa R.
author_sort Scharfstein, Julio
collection PubMed
description Chronic chagasic myocarditis (CCM) depends on Trypanosoma cruzi persistence in the myocardium. Studies of the proteolytic mechanisms governing host/parasite balance in peripheral sites of T. cruzi infection revealed that tissue culture trypomastigotes (TCTs) elicit inflammatory edema and stimulate protective type-1 effector T cells through the activation of the kallikrein-kinin system. Molecular studies linked the proinflammatory phenotype of Dm28c TCTs to the synergistic activities of tGPI, a lipid anchor that functions as a Toll-like receptor 2 (TLR2) ligand, and cruzipain, a kinin-releasing cysteine protease. Analysis of the dynamics of inflammation revealed that TCTs activate innate sentinel cells via TLR2, releasing CXC chemokines, which in turn evoke neutrophil/CXCR2-dependent extravasation of plasma proteins, including high molecular weight kininogen (HK), in parasite-laden tissues. Further downstream, TCTs process surface bound HK, liberating lysyl-BK (LBK), which then propagates inflammatory edema via signaling of endothelial G-protein-coupled bradykinin B(2) receptors (BK(2)R). Dm28 TCTs take advantage of the transient availability of infection-promoting peptides (e.g., bradykinin and endothelins) in inflamed tissues to invade cardiovascular cells via interdependent signaling of BKRs and endothelin receptors (ETRs). Herein we present a space-filling model whereby ceramide-enriched endocytic vesicles generated by the sphingomyelinase pathway might incorporate BK(2)R and ETRs, which then trigger Ca(2+)-driven responses that optimize the housekeeping mechanism of plasma membrane repair from cell wounding. The hypothesis predicts that the NF-κB-inducible BKR (BK(1)R) may integrate the multimolecular signaling platforms forged by ceramide rafts, as the chronic myocarditis progresses. Exploited as gateways for parasite invasion, BK(2)R, BK(1)R, ET(A)R, ET(B)R, and other G protein-coupled receptor partners may enable persistent myocardial parasitism in the edematous tissues at expense of adverse cardiac remodeling.
format Online
Article
Text
id pubmed-3555122
institution National Center for Biotechnology Information
language English
publishDate 2013
publisher Frontiers Media S.A.
record_format MEDLINE/PubMed
spelling pubmed-35551222013-01-25 The kallikrein-kinin system in experimental Chagas disease: a paradigm to investigate the impact of inflammatory edema on GPCR-mediated pathways of host cell invasion by Trypanosoma cruzi Scharfstein, Julio Andrade, Daniele Svensjö, Erik Oliveira, Ana Carolina Nascimento, Clarissa R. Front Immunol Immunology Chronic chagasic myocarditis (CCM) depends on Trypanosoma cruzi persistence in the myocardium. Studies of the proteolytic mechanisms governing host/parasite balance in peripheral sites of T. cruzi infection revealed that tissue culture trypomastigotes (TCTs) elicit inflammatory edema and stimulate protective type-1 effector T cells through the activation of the kallikrein-kinin system. Molecular studies linked the proinflammatory phenotype of Dm28c TCTs to the synergistic activities of tGPI, a lipid anchor that functions as a Toll-like receptor 2 (TLR2) ligand, and cruzipain, a kinin-releasing cysteine protease. Analysis of the dynamics of inflammation revealed that TCTs activate innate sentinel cells via TLR2, releasing CXC chemokines, which in turn evoke neutrophil/CXCR2-dependent extravasation of plasma proteins, including high molecular weight kininogen (HK), in parasite-laden tissues. Further downstream, TCTs process surface bound HK, liberating lysyl-BK (LBK), which then propagates inflammatory edema via signaling of endothelial G-protein-coupled bradykinin B(2) receptors (BK(2)R). Dm28 TCTs take advantage of the transient availability of infection-promoting peptides (e.g., bradykinin and endothelins) in inflamed tissues to invade cardiovascular cells via interdependent signaling of BKRs and endothelin receptors (ETRs). Herein we present a space-filling model whereby ceramide-enriched endocytic vesicles generated by the sphingomyelinase pathway might incorporate BK(2)R and ETRs, which then trigger Ca(2+)-driven responses that optimize the housekeeping mechanism of plasma membrane repair from cell wounding. The hypothesis predicts that the NF-κB-inducible BKR (BK(1)R) may integrate the multimolecular signaling platforms forged by ceramide rafts, as the chronic myocarditis progresses. Exploited as gateways for parasite invasion, BK(2)R, BK(1)R, ET(A)R, ET(B)R, and other G protein-coupled receptor partners may enable persistent myocardial parasitism in the edematous tissues at expense of adverse cardiac remodeling. Frontiers Media S.A. 2013-01-25 /pmc/articles/PMC3555122/ /pubmed/23355836 http://dx.doi.org/10.3389/fimmu.2012.00396 Text en Copyright © Scharfstein, Andrade, Svensjö, Oliveira and Nascimento. http://creativecommons.org/licenses/by/3.0/ This is an open-access article distributed under the terms of the Creative Commons Attribution License, which permits use, distribution and reproduction in other forums, provided the original authors and source are credited and subject to any copyright notices concerning any third-party graphics etc.
spellingShingle Immunology
Scharfstein, Julio
Andrade, Daniele
Svensjö, Erik
Oliveira, Ana Carolina
Nascimento, Clarissa R.
The kallikrein-kinin system in experimental Chagas disease: a paradigm to investigate the impact of inflammatory edema on GPCR-mediated pathways of host cell invasion by Trypanosoma cruzi
title The kallikrein-kinin system in experimental Chagas disease: a paradigm to investigate the impact of inflammatory edema on GPCR-mediated pathways of host cell invasion by Trypanosoma cruzi
title_full The kallikrein-kinin system in experimental Chagas disease: a paradigm to investigate the impact of inflammatory edema on GPCR-mediated pathways of host cell invasion by Trypanosoma cruzi
title_fullStr The kallikrein-kinin system in experimental Chagas disease: a paradigm to investigate the impact of inflammatory edema on GPCR-mediated pathways of host cell invasion by Trypanosoma cruzi
title_full_unstemmed The kallikrein-kinin system in experimental Chagas disease: a paradigm to investigate the impact of inflammatory edema on GPCR-mediated pathways of host cell invasion by Trypanosoma cruzi
title_short The kallikrein-kinin system in experimental Chagas disease: a paradigm to investigate the impact of inflammatory edema on GPCR-mediated pathways of host cell invasion by Trypanosoma cruzi
title_sort kallikrein-kinin system in experimental chagas disease: a paradigm to investigate the impact of inflammatory edema on gpcr-mediated pathways of host cell invasion by trypanosoma cruzi
topic Immunology
url https://www.ncbi.nlm.nih.gov/pmc/articles/PMC3555122/
https://www.ncbi.nlm.nih.gov/pubmed/23355836
http://dx.doi.org/10.3389/fimmu.2012.00396
work_keys_str_mv AT scharfsteinjulio thekallikreinkininsysteminexperimentalchagasdiseaseaparadigmtoinvestigatetheimpactofinflammatoryedemaongpcrmediatedpathwaysofhostcellinvasionbytrypanosomacruzi
AT andradedaniele thekallikreinkininsysteminexperimentalchagasdiseaseaparadigmtoinvestigatetheimpactofinflammatoryedemaongpcrmediatedpathwaysofhostcellinvasionbytrypanosomacruzi
AT svensjoerik thekallikreinkininsysteminexperimentalchagasdiseaseaparadigmtoinvestigatetheimpactofinflammatoryedemaongpcrmediatedpathwaysofhostcellinvasionbytrypanosomacruzi
AT oliveiraanacarolina thekallikreinkininsysteminexperimentalchagasdiseaseaparadigmtoinvestigatetheimpactofinflammatoryedemaongpcrmediatedpathwaysofhostcellinvasionbytrypanosomacruzi
AT nascimentoclarissar thekallikreinkininsysteminexperimentalchagasdiseaseaparadigmtoinvestigatetheimpactofinflammatoryedemaongpcrmediatedpathwaysofhostcellinvasionbytrypanosomacruzi
AT scharfsteinjulio kallikreinkininsysteminexperimentalchagasdiseaseaparadigmtoinvestigatetheimpactofinflammatoryedemaongpcrmediatedpathwaysofhostcellinvasionbytrypanosomacruzi
AT andradedaniele kallikreinkininsysteminexperimentalchagasdiseaseaparadigmtoinvestigatetheimpactofinflammatoryedemaongpcrmediatedpathwaysofhostcellinvasionbytrypanosomacruzi
AT svensjoerik kallikreinkininsysteminexperimentalchagasdiseaseaparadigmtoinvestigatetheimpactofinflammatoryedemaongpcrmediatedpathwaysofhostcellinvasionbytrypanosomacruzi
AT oliveiraanacarolina kallikreinkininsysteminexperimentalchagasdiseaseaparadigmtoinvestigatetheimpactofinflammatoryedemaongpcrmediatedpathwaysofhostcellinvasionbytrypanosomacruzi
AT nascimentoclarissar kallikreinkininsysteminexperimentalchagasdiseaseaparadigmtoinvestigatetheimpactofinflammatoryedemaongpcrmediatedpathwaysofhostcellinvasionbytrypanosomacruzi

Ejemplares similares