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    Por favor, use este identificador para citar o enlazar este ítem:https://uvadoc.uva.es/handle/10324/55178

    Título
    Treatment with bortezomib of human CD4+ T cells preserves natural regulatory T cells and allows the emergence of a distinct suppressor T-cell population
    Autor
    Blanco Durango, Belén
    Perez Simon, José Antonio
    Sánchez Abarca, Luis Ignacio
    Caballero Velazquez, Teresa
    Gutierrez Cossio, Silvia
    Hernández Campo, Pilar
    Diez Campelo, María
    Herrero Sánchez, María del CarmenAutoridad UVA
    Rodríguez Serrano, Concepción
    Santamaría Quesada, Carlos
    Sánchez Guijo, Fermín
    Cañizo Fernández-Roldán, Consuelo del
    San Miguel Izquierdo, Jesús F.
    Año del Documento
    2009
    Editorial
    Ferrata Storti Foundation
    Descripción
    Producción Científica
    Documento Fuente
    Haematologica, 2009, Vol. 94, Nº. 7, págs. 975-983
    Resumo
    Background In vitro depletion of alloreactive T cells using the proteasome inhibitor bortezomib is a promising approach to prevent graft-versus-host disease after allogeneic stem cell transplantation. We have previously described the ability of bortezomib to selectively eliminate alloreactive T cells in a mixed leukocyte culture, preserving non-activated T cells. Due to the role of regulatory T cells in the control of graft versus host disease, in the current manuscript we have analyzed the effect of bortezomib in regulatory T cells.Design and Methods Conventional or regulatory CD4+ T cells were isolated with immunomagnetic microbeads based on the expression of CD4 and CD25. The effect of bortezomib on T-cell viability was analyzed by flow cytometry using 7-amino-actinomycin D staining. To investigate the possibility of obtaining an enriched regulatory T-cell population in vitro with the use of bortezomib, CD4+ T cells were cultured during four weeks in the presence of anti-CD3 and anti-CD28 antibodies, IL-2 and bortezomib. The phenotype of these long-term cultured cells was studied, analyzing the expression of CD25, CD127 and FOXP3 by flow cytometry, and mRNA levels were determined by RT-PCR. Their suppressive capacity was assessed in co-culture experiments, analyzing proliferation and IFN-γ and CD40L expression of stimulated responder T cells by flow cytometry.Results We observed that naturally occurring CD4+CD25+ regulatory T cells are resistant to the pro-apoptotic effect of bortezomib. Furthermore, we found that long-term culture of CD4+ T cells in the presence of bortezomib promotes the emergence of a regulatory T-cell population that significantly inhibits proliferation, IFN-γ production and CD40L expression among stimulated effector T cells.Conclusions These results reinforce the proposal of using bortezomib in the prevention of graft versus host disease and, moreover, in the generation of regulatory T-cell populations, that could be used in the treatment of multiple T-cell mediated diseases.
    Materias (normalizadas)
    Cell Biology
    Graft versus host disease
    Cell transplantation
    Trasplante de células
    Medical microbiology
    Pharmacology
    Materias Unesco
    3205.04 Hematología
    3207.13 Oncología
    ISSN
    0390-6078
    Revisión por pares
    SI
    DOI
    10.3324/haematol.2008.005017
    Version del Editor
    https://haematologica.org/article/view/5306
    Propietario de los Derechos
    © Ferrata Storti Foundation
    Idioma
    eng
    URI
    https://uvadoc.uva.es/handle/10324/55178
    Tipo de versión
    info:eu-repo/semantics/publishedVersion
    Derechos
    openAccess
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    • DEP06 - Artículos de revista [353]
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    Universidad de Valladolid

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