2015
DOI: 10.1128/mcb.00706-15
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Histone Deacetylase 3 Is Required for Efficient T Cell Development

Abstract: Hdac3 is a key target for Hdac inhibitors that are efficacious in cutaneous T cell lymphoma. Moreover, the regulation of chromatin structure is critical as thymocytes transition from an immature cell with open chromatin to a mature T cell with tightly condensed chromatin. To define the phenotypes controlled by Hdac3 during T cell development, we conditionally deleted Hdac3 using the Lck-Cre transgene. This strategy inactivated Hdac3 in the double-negative stages of thymocyte development and caused a significan… Show more

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Cited by 45 publications
(49 citation statements)
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“…However various aspects are different from our work, including that the block in positive selection was due to a defect in gene regulation that could be bypassed by a strong TCR signaling with an OT-II TCR transgene (51). Differences observed between both studies may stem from the mouse models utilized, where Stengal et al used an Lck-cre for HDAC3 elimination compared to CD2-icre in our work.…”
Section: Discussioncontrasting
confidence: 72%
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“…However various aspects are different from our work, including that the block in positive selection was due to a defect in gene regulation that could be bypassed by a strong TCR signaling with an OT-II TCR transgene (51). Differences observed between both studies may stem from the mouse models utilized, where Stengal et al used an Lck-cre for HDAC3 elimination compared to CD2-icre in our work.…”
Section: Discussioncontrasting
confidence: 72%
“…However, we demonstrate that the key gene downstream of HDAC3 required for positive selection is RORγt, as protein levels were not reduced with positive selection and CD8SP thymocyte development was restored to WT levels in RB3 mice. RORC mRNA levels were also increased in DP thymocytes from Lck-cre HDAC3-cKO mice examined by Stengel et al (51). As few CD4SP thymocytes developed in RB3 mice, HDAC3 might play an additional role in thymocyte development during CD4-lineage choice.…”
Section: Discussionmentioning
confidence: 78%
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“…However, there were also defects in the formation of the earliest lymphoid-primed multipotent progenitor cells, suggesting a more complex mechanism underlying the role of Hdac3 in lymphoid development (10). Deletion of Hdac3 in early T cells also caused a lack of cell survival and impaired differentiation, but deletion later in development caused only functional defects (37)(38)(39). Here, deletion of Hdac3 in early committed B progenitor cells uncovered unexpected roles for Hdac3 in yielding productive VDJ recombination.…”
Section: Discussionmentioning
confidence: 86%