Recombinant vaccines of a CD4+ T-cell epitope promote efficient control of Paracoccidioides brasiliensis burden by restraining primary organ infection

dc.creatorAlves Santos, Julliana Ribeiro
dc.creatorAssuncão Holanda, Rodrigo
dc.creatorMuñoz, J.E.
dc.creatorSantos Dias, Lucas
dc.creatorRoque Silva, Leandro Buffoni
dc.creatorAlves Santos, Julliana Ribeiro
dc.creatorPagliari, Sthefany
dc.creatorLeandro, Érica
dc.creatorVieira, Marciano
dc.creatorAlves Paixão, Tatiane
dc.creatorPelleschi Taborda, Carlos
dc.creatorAssis Santos, Daniel
dc.creatorBruña-Romero, Oscar
dc.date.accessioned2018-11-06T17:50:12Z
dc.date.available2018-11-06T17:50:12Z
dc.date.created2018-11-06T17:50:12Z
dc.date.issued2017
dc.identifierISSN 1935-2727
dc.identifierISSNe 1935-2735
dc.identifierhttp://repository.urosario.edu.co/handle/10336/18682
dc.identifierhttps://doi.org/10.1371/journal.pntd.0005927
dc.description.abstractParacoccidioidomycosis (PCM) is an infectious disease endemic to South America, caused by the thermally dimorphic fungi Paracoccidioides. Currently, there is no effective human vaccine that can be used in prophylactic or therapeutic regimes. We tested the hypothesis that the immunogenicity of the immunodominant CD4+T-cell epitope (P10) of Paracoccidioides brasiliensis gp43 antigen might be significantly enhanced by using a hepatitis B virus-derived particle (VLP) as an antigen carrier. This chimera was administered to mice as a (His)6-purified protein (rPbT) or a replication-deficient human type 5 adenoviral vector (rAdPbT) in an immunoprophylaxis assay. The highly virulent Pb18 yeast strain was used to challenge our vaccine candidates. Fungal challenge evoked robust P10-specific memory CD4+T cells secreting protective Th-1 cytokines in most groups of immunized mice. Furthermore, the highest level of fungal burden control was achieved when rAdPbT was inoculated in a homologous prime-boost regimen, with 10-fold less CFU recovering than in non-vaccinated mice. Systemic Pb18 spreading was only prevented when rAdPbT was previously inoculated. In summary, we present here VLP/P10 formulations as vaccine candidates against PCM, some of which have demonstrated for the first time their ability to prevent progression of this pernicious fungal disease, which represents a significant social burden in developing countries. © 2017 Holanda et al.
dc.languageeng
dc.relationPLoS Neglected Tropical Diseases, ISSN 1935-2727, Vol. 11 No. 9 (2017)
dc.relationhttps://journals.plos.org/plosntds/article/file?id=10.1371/journal.pntd.0005927&type=printable
dc.relationNo. 9
dc.relationPLoS Neglected Tropical Diseases
dc.relationVol. 11
dc.rights
dc.rightsinfo:eu-repo/semantics/openAccess
dc.rightsAbierto (Texto Completo)
dc.rightshttps://creativecommons.org/licenses/by/4.0/
dc.sourceMunoz, J.F., Gallo, J.E., Misas, E., Priest, M., Imamovic, A., Young, S., Genome update of the dimorphic human pathogenic fungi causing paracoccidioidomycosis (2014) Plos Neglect Trop D, 8, p. e3348
dc.sourceinstname:Universidad del Rosario
dc.sourcereponame:Repositorio Institucional EdocUR
dc.subjectEpítopo
dc.subjectPartícula similar a un virus
dc.subjectInterferón gamma
dc.subjectHongos
dc.subjectSintético
dc.subjectLinfocito T
dc.subjectBalb endogámico C
dc.subjectParacoccidioides
dc.subjectDesarrollo y Envejecimiento
dc.subjectVacuna
dc.subjectInterleucina 1
dc.subjectinterleucina 12
dc.subjectinterleucina 4
dc.subjectVacuna recombinante
dc.subjectFactor de necrosis tumoral
dc.subjectProteína de 43 Kda
dc.subjectCitocina
dc.subjectEpítopo
dc.subjectProteína fúngica
dc.subjectAntígeno de hongos
dc.subjectVacuna contra hongos
dc.subjectGlicoproteína
dc.subjectVacuna recombinante
dc.subjectVacuna contra partículas similares a virus
dc.subjectCélula animal
dc.subjectExperimento con animales
dc.subjectModelo animal
dc.subjectTejido animal
dc.subjectLinfocito T Cd4+
dc.subjectInmunidad celular
dc.subjectCentrifugación
dc.subjectQuimera
dc.subjectUnidad de formación de Colonia
dc.subjectEstudio controlado
dc.subjectReplicación de ADN
dc.subjectFormulación de Medicamentos
dc.subjectEnsayo inmunoabsorbente ligado a enzimas
dc.subjectHepatitis B
dc.subjectHistopatología
dc.subjectHumano
dc.subjectCélula humana
dc.subjectInmunización
dc.subjectInmunofenotipado
dc.subjectInmunoprofilaxis
dc.subjectProliferación de linfocitos
dc.subjectMétodo de estimación de la magnitud
dc.subjectMortalidad
dc.subjectSíntesis de péptidos
dc.subjectPlásmido
dc.subjectElectroforesis en gel de poliacrilamida
dc.subjectExpresión de proteínas
dc.subjectExtracción de fase sólida
dc.subjectBlastomicosis sudamericana
dc.subjectLesión de tejido
dc.subjectMicroscopio de transmisión por electrones
dc.subjectInmunogenicidad de la vacuna
dc.subjectPartícula de virus
dc.subjectTransferencia occidental
dc.subjectRatón albino bagg
dc.subjectGenética
dc.subjectCrecimiento
dc.subjectHepatitis B Virus
dc.subjectMemoria Inmunológica
dc.subjectInmunología
dc.subjectMicrobiología
dc.subjectParacoccidioides
dc.subjectParacoccidioidomicosis
dc.subjectSecreción (Proceso)
dc.subjectCélula Th1
dc.titleRecombinant vaccines of a CD4+ T-cell epitope promote efficient control of Paracoccidioides brasiliensis burden by restraining primary organ infection
dc.typearticle


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