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Direct BMP2/4 signaling through BMP receptor IA regulates fetal thymocyte progenitor homeostasis and differentiation to CD4+CD8+ double-positive cell

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dc.contributor.author Hager-Theodorides, AL en
dc.contributor.author Ross, SE en
dc.contributor.author Sahni, H en
dc.contributor.author Mishina, Y en
dc.contributor.author Furmanski, AL en
dc.contributor.author Crompton, T en
dc.date.accessioned 2014-06-06T06:53:01Z
dc.date.available 2014-06-06T06:53:01Z
dc.date.issued 2014 en
dc.identifier.issn 15384101 en
dc.identifier.uri http://dx.doi.org/10.4161/cc.27118 en
dc.identifier.uri http://62.217.125.90/xmlui/handle/123456789/6310
dc.subject Alk3 en
dc.subject BMP2/4 en
dc.subject BMPRIA en
dc.subject Differentiation en
dc.subject DN thymocyte en
dc.subject DP en
dc.subject Noggin en
dc.subject Smad en
dc.subject T-cell development en
dc.subject Thymus en
dc.subject.other bone morphogenetic protein 2 en
dc.subject.other bone morphogenetic protein 4 en
dc.subject.other bone morphogenetic protein receptor 1A en
dc.subject.other article en
dc.subject.other CD4 CD8 ratio en
dc.subject.other cell differentiation en
dc.subject.other cell lineage en
dc.subject.other ex vivo study en
dc.subject.other excision en
dc.subject.other homeostasis en
dc.subject.other mouse en
dc.subject.other nonhuman en
dc.subject.other T lymphocyte en
dc.subject.other thymocyte en
dc.subject.other thymus en
dc.title Direct BMP2/4 signaling through BMP receptor IA regulates fetal thymocyte progenitor homeostasis and differentiation to CD4+CD8+ double-positive cell en
heal.type journalArticle en
heal.identifier.primary 10.4161/cc.27118 en
heal.publicationDate 2014 en
heal.abstract BMP2/4 signaling is required for embryogenesis and involved in thymus morphogenesis and T-lineage differentiation. In vitro experiments have shown that treatment of thymus explants with exogenous BMP4 negatively regulated differentiation of early thymocyte progenitors and the transition from CD4-CD8- (DN) to CD4+CD8+ (DP). Here we show that in vivo BMP2/4 signaling is required for fetal thymocyte progenitor homeostasis and expansion, but negatively regulates differentiation from DN to DP cell. Unexpectedly, conditional deletion of BMPRIA from fetal thymocytes (using the Cre-loxP system and directing excision to hematopoietic lineage cells with the Vav promoter) demonstrated that physiological levels of BMP2/4 signaling directly to thymocytes through BMPRIA are required for normal differentiation and expansion of early fetal DN thymocytes. In contrast, the arrest in early thymocyte progenitor differentiation caused by exogenous BMP4 treatment of thymus explants is induced in part by direct signaling to thymocytes through BMPRIA, and in part by indirect signaling through non-hematopoietic cells. Analysis of the transition from fetal DN to DP cell, both by ex vivo analysis of conditional BMPRIA-deficient thymocytes and by treatment of thymus explants with the BMP4- inhibitor Noggin demonstrated that BMP2/4 signaling is a negative regulator at this stage. We showed that at this stage of fetal T-cell development BMP2/4 signals directly to thymocytes through BMPRIA. © 2014 Landes Bioscience. en
heal.journalName Cell Cycle en
dc.identifier.issue 2 en
dc.identifier.volume 13 en
dc.identifier.doi 10.4161/cc.27118 en
dc.identifier.spage 324 en
dc.identifier.epage 333 en


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