2015
DOI: 10.1128/jvi.03076-14
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Constitutive but Not Inducible Attenuation of Transforming Growth Factor β Signaling Increases Natural Killer Cell Responses without Directly Affecting Dendritic Cells Early after Persistent Viral Infection

Abstract: Rapid innate responses to viral encounters are crucial to shaping the outcome of infection, from viral clearance to persistence. Transforming growth factor ␤ (TGF-␤) is a potent immune suppressor that is upregulated early upon viral infection and maintained during chronic infections in both mice and humans. However, the role of TGF-␤ signaling in regulating individual cell types in vivo is still unclear. Using infections with two different persistent viruses, murine cytomegalovirus (MCMV) and lymphocytic chori… Show more

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Cited by 5 publications
(7 citation statements)
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References 72 publications
(147 reference statements)
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“…By using inducible Tgfbr2 deletion in adult mice, we extend the aforementioned CD8 T cell findings showing that TGFβ-RII signaling (after) infection negligibly influenced endogenous polyclonal CD8 T cells responses, both early and late during chronic LCMV or MCMV infections. Similarly, we recently used both cell type-specific and the inducible ERCre Tgfbr2 deletion system to demonstrate that TGFβ-RII signaling does not significantly influence early NK or dendritic cell responses to systemic chronic LCMV or MCMV infections in vivo (50). These observations are particularly striking given the long-appreciated exogenous TGF-β-mediated suppression of cytotoxic NK, dendritic cell, and CD8 T cell responses in vitro and/or during in vivo viral infection (51-53).…”
Section: Discussionmentioning
confidence: 99%
“…By using inducible Tgfbr2 deletion in adult mice, we extend the aforementioned CD8 T cell findings showing that TGFβ-RII signaling (after) infection negligibly influenced endogenous polyclonal CD8 T cells responses, both early and late during chronic LCMV or MCMV infections. Similarly, we recently used both cell type-specific and the inducible ERCre Tgfbr2 deletion system to demonstrate that TGFβ-RII signaling does not significantly influence early NK or dendritic cell responses to systemic chronic LCMV or MCMV infections in vivo (50). These observations are particularly striking given the long-appreciated exogenous TGF-β-mediated suppression of cytotoxic NK, dendritic cell, and CD8 T cell responses in vitro and/or during in vivo viral infection (51-53).…”
Section: Discussionmentioning
confidence: 99%
“…(Allen et al, 2011; Lewis et al, 2015;Marcoe et al, 2012) dLck-TGF-bRII Deleción constitutiva tardía del TGFbRII en LT Deficiencia en el desarrollo de LT intestinales específicos de LCMV y de LThf específicos de influenza en pulmón. (Marshall et al, 2015;Sheridan et al, 2014;Zhang and Bevan, 2013) ERcre-TGF-bRII Deleción inducible del TGF-bRII en todas las células La atenuación de la señalización del TGF-β no afecta las CD y NK y su capacidad par eliminar la infección aguda de MCMV y la crónica de LCMV.…”
Section: Cd4dntgf-briiunclassified
“…( Lewis et al, 2015) dominante negativa del TGF-βRII en dichas células. En estos ratones se evidencia una disminución del número y función de las NK pero no de las CD y se atenúa la eliminación del virus Herpes y el citomegalovirus murino (MCMV), pero no la infección crónica con LCMV (Allen, et al Para tratar de evitar el problema de la alteración celular que ocurre en los ratones genéticamente modificados constitutivamente, recientemente se recurrió a ratones ERcre-TGF-βRII que al ser tratados con tamoxifeno tienen una deleción inducible del TGF-βRII en todas las células del organismo.…”
Section: Cd4dntgf-briiunclassified
See 1 more Smart Citation
“…For instance, epigenetic changes induced by tumor-driven metabolic restrictions suppress T-cell activity (Zhao et al, 2016). In addition, TGF-β, an immunosuppressive mediator expressed at high levels in most established malignancies, does not play a crucial role in the pathogenesis of many viral infections (Flavell et al, 2010; Furuya et al, 2015; Garidou et al, 2012; Lewis et al, 2015; Wrzesinski et al, 2007). Thus, tumors induce dendritic cells (DCs), as well as conventional and regulatory T (Treg) cells to secrete TGF-β, which impairs effector T-cell activity through multiple mechanisms that include Foxp1-mediated transcriptional repression (Stephen et al, 2014) and suppression of effector cytokines (Ahmadzadeh and Rosenberg, 2005).…”
Section: Introductionmentioning
confidence: 99%