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dc.contributor.author VAZQUEZ CHAGOYAN, JUAN CARLOS
dc.contributor.author Garg, Nisha
dc.contributor.author Gupta, Shivali
dc.contributor.author SALGADO JIMENEZ, BERENICE
dc.contributor.author Lokugamage, Nandadeva
dc.creator VAZQUEZ CHAGOYAN, JUAN CARLOS; 120705
dc.creator Garg, Nisha;#0000-0002-3453-2369
dc.creator Gupta, Shivali;#0000-0002-9598-7965
dc.creator SALGADO JIMENEZ, BERENICE; 216840
dc.creator Lokugamage, Nandadeva;#0000-0001-8734-6538
dc.date.accessioned 2020-02-28T21:39:43Z
dc.date.available 2020-02-28T21:39:43Z
dc.date.issued 2019-06-26
dc.identifier.issn 1664-3224
dc.identifier.uri http://hdl.handle.net/20.500.11799/106037
dc.description Artículo Científico es
dc.description.abstract Background: Chagas cardiomyopathy is caused by Trypanosoma cruzi (Tc). Two antigenic candidates, TcG2 and TcG4, are recognized by antibodies in naturally infected dogs and humans; and these vaccine candidates provided protection from Tc infection in mice and dogs. Trypanosoma rangeli (Tr) is non-pathogenic to mammals and shown to elicit cross-reactive anti-Tc antibodies. In this study, we investigated if fixed Tr (fTr) can further enhance the efficacy of the TcG2/TcG4 DNA vaccine. Methods and Results: C57BL/6 mice were immunized with TcG2/TcG4 DNA vaccine and fTr (delivered as an adjuvant or in prime-boost approach), and challenged with Tc. Serology studies showed that fTr (±quil-A) elicited Tc- and Tr-reactive IgGs that otherwise were not stimulated by TcG2/TcG4 vaccine only, and quil-A had suppressive effects on fTr-induced IgGs. After challenge infection, TcG2/TcG4-vaccinated mice exhibited potent expansion of antigen- and Tc-specific IgGs that were not boosted by fTr±quil-A. Flow cytometry analysis showed that TcG2/TcG4-induced dendritic cells (DC) and macrophages (M0) responded to challenge infection by expression of markers of antigen uptake, processing, and presentation, and production of pro-inflammatory cytokines. TcG2/TcG4-induced CD4+T cells acquired Th1 phenotype and expressed markers that orchestrate adaptive immunity. A fraction of vaccine-induced CD4+T cells exhibited iTreg phenotype responsible for aversion of self-injurious immune responses. Further, TcG2/TcG4-vaccinated mice exhibited potent expansion of poly-functional CD8+T cells with TNF-a/IFN-g production and cytolytic phenotype post-infection. Subsequently, tissue parasites and pathology were hardly detectable in TcG2/TcG4-vaccinated/infected mice. Inclusion of fTr±quil-A had no clear additive effects in improving the Tc-specific adaptive immunity and parasite control than was noted in mice vaccinated with TcG2/TcG4 alone. Non-vaccinated Gupta et al. Vaccine Testing Against T. cruzi mice lacked sufficient activation of Th1 CD4+/CD8+T cells, and exhibited >10-fold higher levels of tissue parasite burden than was noted in vaccinated/infected mice. Conclusion: TcG2/TcG4 vaccine elicits highly effective immunity, and inclusion of fTr is not required to improve the efficacy of DNA vaccine against acute Tc infection in mice. es
dc.description.sponsorship UTMB es
dc.language.iso eng es
dc.publisher Frontiers in immunology es
dc.rights openAccess es
dc.rights.uri http://creativecommons.org/licenses/by-nc-nd/4.0
dc.subject Trypanosoma cruzi es
dc.subject Chagas Disease es
dc.subject Recombinant DNA Vaccine es
dc.subject T. rangeli es
dc.subject immune efficacy es
dc.subject.classification MEDICINA Y CIENCIAS DE LA SALUD
dc.title TcG2/TcG4 DNA Vaccine Induces Th1 Immunity Against Acute Trypanosoma cruzi Infection: Adjuvant and Antigenic Effects of Heterologous T. rangeli Booster Immunization es
dc.type Artículo es
dc.provenance Científica es
dc.road Dorada es
dc.organismo Medicina Veterinaria y Zootecnia es
dc.ambito Internacional es
dc.cve.CenCos 21401 es
dc.modalidad Artículo especializado para publicar en revista indizada es
dc.audience students es
dc.audience researchers es
dc.type.conacyt article
dc.identificator 3
dc.relation.vol 10
dc.relation.año 2019
dc.relation.no 1456
dc.relation.doi 10.3389/fimmu.2019.01456


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  • Título
  • TcG2/TcG4 DNA Vaccine Induces Th1 Immunity Against Acute Trypanosoma cruzi Infection: Adjuvant and Antigenic Effects of Heterologous T. rangeli Booster Immunization
  • Autor
  • VAZQUEZ CHAGOYAN, JUAN CARLOS
  • Garg, Nisha
  • Gupta, Shivali
  • SALGADO JIMENEZ, BERENICE
  • Lokugamage, Nandadeva
  • Fecha de publicación
  • 2019-06-26
  • Editor
  • Frontiers in immunology
  • Tipo de documento
  • Artículo
  • Palabras clave
  • Trypanosoma cruzi
  • Chagas Disease
  • Recombinant DNA Vaccine
  • T. rangeli
  • immune efficacy
  • Los documentos depositados en el Repositorio Institucional de la Universidad Autónoma del Estado de México se encuentran a disposición en Acceso Abierto bajo la licencia Creative Commons: Atribución-NoComercial-SinDerivar 4.0 Internacional (CC BY-NC-ND 4.0)

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