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AuthorMelo, Andréa Barbosa de
AuthorNascimento, Eduardo J. M.
AuthorBraga-Neto, Ulisses
AuthorDhalia, Rafael
AuthorSilva, Ana Maria
AuthorOelke, Mathias
AuthorSchneck, Jonathan P.
AuthorSidney, John
AuthorSette, Alessandro
AuthorMontenegro, Silvia M. L.
AuthorMarques, Ernesto T. A.
Access date2017-12-15T13:01:30Z
Available date2017-12-15T13:01:30Z
Document date2013
CitationMELO, A. B. de et al. T-cell memory responses elicited by yellow fever vaccine are targeted to overlapping epitopes containing multiple HLA-I and -II binding motifs. PLoS neglected tropical diseases, v. 7, n. 1, p. e1938, 2013.pt_BR
ISSN1935-2735pt_BR
URIhttps://www.arca.fiocruz.br/handle/icict/23667
SponsorshipEste trabalho foi apoiado pela Subvenção AI-40085 dos Institutos Nacionais de Saúde; Fundação Oswaldo Cruz, PDTIS- RVR9; Conselho Nacional de Desenvolvimento Científico e Tecnológico (CNPq); Fundação Nacional da Ciência, CCF-0845407; e o Conselho Brasileiro de Ensino Superior (CAPES), bolsa de doutorado da AB). Os financiadores não tiveram papel em design de estudo, coleta e análise de dados, decisão de publicação ou preparação do manuscrito.pt_BR
Languageengpt_BR
PublisherAlan L. Rothmanpt_BR
Rightsopen accesspt_BR
Subject in PortugueseFebre Amarelapt_BR
Subject in Portuguesecitologiapt_BR
Subject in PortugueseVacinaspt_BR
Subject in PortugueseCD4pt_BR
TitleT-cell memory responses elicited by yellow fever vaccine are targeted to overlapping epitopes containing multiple HLA-I and -II binding motifspt_BR
TypeArticlept_BR
DOI10.1371/journal.pntd.0001938
AbstractThe yellow fever vaccines (YF-17D-204 and 17DD) are considered to be among the safest vaccines and the presence of neutralizing antibodies is correlated with protection, although other immune effector mechanisms are known to be involved. T-cell responses are known to play an important role modulating antibody production and the killing of infected cells. However, little is known about the repertoire of T-cell responses elicited by the YF-17DD vaccine in humans. In this report, a library of 653 partially overlapping 15-mer peptides covering the envelope (Env) and nonstructural (NS) proteins 1 to 5 of the vaccine was utilized to perform a comprehensive analysis of the virus-specific CD4(+) and CD8(+) T-cell responses. The T-cell responses were screened ex-vivo by IFN-γ ELISPOT assays using blood samples from 220 YF-17DD vaccinees collected two months to four years after immunization. Each peptide was tested in 75 to 208 separate individuals of the cohort. The screening identified sixteen immunodominant antigens that elicited activation of circulating memory T-cells in 10% to 33% of the individuals. Biochemical in-vitro binding assays and immunogenetic and immunogenicity studies indicated that each of the sixteen immunogenic 15-mer peptides contained two or more partially overlapping epitopes that could bind with high affinity to molecules of different HLAs. The prevalence of the immunogenicity of a peptide in the cohort was correlated with the diversity of HLA-II alleles that they could bind. These findings suggest that overlapping of HLA binding motifs within a peptide enhances its T-cell immunogenicity and the prevalence of the response in the population. In summary, the results suggests that in addition to factors of the innate immunity, "promiscuous" T-cell antigens might contribute to the high efficacy of the yellow fever vaccines.pt_BR
AffilliationFundação Oswaldo Cruz. Instituto Aggeu Magalhães. Laboratório de Virologia e Terapia Experimental. Recife, PE, Brasil.pt_BR
AffilliationUniversity of Pittsburgh. Center for Vaccine Research. Department of Infectious Diseases and Microbiology. Pittsburgh, Pennsylvania, United States of America.pt_BR
AffilliationTexas A&M University. College Station. Department of Electrical and Computer Engineering. Texas, United States of America.pt_BR
AffilliationFundação Oswaldo Cruz. Instituto Aggeu Magalhães. Laboratório de Virologia e Terapia Experimental. Recife, PE, Brasil.pt_BR
AffilliationFundação Oswaldo Cruz. Instituto Aggeu Magalhães. Laboratório de Virologia e Terapia Experimental. Recife, PE, Brasil.pt_BR
AffilliationThe Johns Hopkins University School of Medicine. Department of Pathology. Baltimore, Maryland, United States of America.pt_BR
AffilliationThe Johns Hopkins University School of Medicine. Department of Pathology. Baltimore, Maryland, United States of America.pt_BR
AffilliationLa Jolla Institute for Allergy and Immunology. Vaccine Discovery. La Jolla, California, United States of America.pt_BR
AffilliationLa Jolla Institute for Allergy and Immunology. Vaccine Discovery. La Jolla, California, United States of America.pt_BR
AffilliationFundação Oswaldo Cruz. Instituto Aggeu Magalhães. Departamento de imunologia. Recife, PE, Brasil.pt_BR
AffilliationFundação Oswaldo Cruz. Instituto Aggeu Magalhães. Laboratório de Virologia e Terapia Experimental. Recife, PE, Brasil / University of Pittsburgh. Center for Vaccine Research. Department of Infectious Diseases and Microbiology. Pittsburgh, Pennsylvania, United States of America.pt_BR
Subjectyellow feverpt_BR
Subjectcytologypt_BR
SubjectVaccinept_BR
SubjectCD4pt_BR
DeCSEpitopos de Linfócito Tpt_BR
DeCSimunologiapt_BR
DeCSAntígenos de Histocompatibilidade Classe IIpt_BR
DeCSimunologiapt_BR
DeCSAntígenos de Histocompatibilidade Classe Ipt_BR
DeCSimunologiapt_BR
DeCSMemória Imunológicapt_BR
DeCSHumanospt_BR
DeCSLinfócitos Tpt_BR
DeCSimunologiapt_BR
DeCSVacina contra Febre Amarelapt_BR
DeCSimunologiapt_BR
DeCSInterferon gamapt_BR
DeCSsecreçãopt_BR
DeCSVacina contra Febre Amarelapt_BR
DeCSadministração & dosagempt_BR
DeCSELISPOTpt_BR
xmlui.metadata.dc.subject.ods03 Saúde e Bem-Estar


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