The chromatin-remodeling enzyme BRG1 plays an essential role in primitive erythropoiesis and vascular development

Griffin, Courtney T.; Brennan, Jennifer; Magnuson, Terry

doi:10.1242/dev.010090

Cited by 117 publications

(127 citation statements)

References 41 publications

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“…Therefore, one outstanding issue is whether BRG1 differentially impacts the timing and location of COUP-TFII expression in developing vasculature. This research article demonstrates that BRG1 promotes venous COUP-TFII expression during early stages of vascular development, but it is not clear whether BRG1 is required for COUP-TFII maintenance on more mature veins, as Brg1 fl/fl :Tie2-Cre + embryos die from anemia by E11.0 (Griffin et al, 2008). To address this issue, vascular Brg1 excision must be induced at later stages of embryonic development.…”

Section: Development 140 (6)mentioning

confidence: 99%

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BRG1 promotesCOUP-TFIIexpression and venous specification during embryonic vascular development

2013

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SUMMARYArteries and veins acquire distinct molecular identities prior to the onset of embryonic blood circulation, and their specification is crucial for vascular development. The transcription factor COUP-TFII currently functions at the top of a signaling pathway governing venous fate. It promotes venous identity by inhibiting Notch signaling and subsequent arterialization of endothelial cells, yet nothing is known about what regulates COUP-TFII expression in veins. We now report that the chromatin-remodeling enzyme BRG1 promotes COUP-TFII expression in venous endothelial cells during murine embryonic development. Conditional deletion of Brg1 from vascular endothelial cells resulted in downregulated COUP-TFII expression and aberrant expression of arterial markers on veins. BRG1 promotes COUP-TFII expression by binding conserved regulatory elements within the COUP-TFII promoter and remodeling chromatin to make the promoter accessible to transcriptional machinery. This study provides the first description of a factor promoting COUP-TFII expression in vascular endothelium and highlights a novel role for chromatin remodeling in venous specification.

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Section: Development 140 (6)mentioning

confidence: 99%

“…Tissues were fixed in a 2% PFA/0.2% glutaraldehyde solution, washed and X-gal stained as described (Griffin et al, 2008) for 48 hours at room temperature. The stained yolk sacs were dissected away from embryos and placentae and flat-mounted in DABCO mounting media on glass slides as described above.…”

Section: Whole-mount Yolk Sac and Placental Stainingmentioning

confidence: 99%

BRG1 promotesCOUP-TFIIexpression and venous specification during embryonic vascular development

2013

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“…For example, BAF complex subunits have specific and important roles in maintaining hematopoietic stem cells (HSCs), the stem cells that give rise to all cellular components of blood (Krasteva et al, 2012). They also control the differentiation of HSCs to different lineages (Bultman et al, 2005;Griffin et al, 2008;Vradii et al, 2006) and, subsequently, different stages of B-and Tcell development.…”

Section: Roles For Baf Complexes During Immune Cell Developmentmentioning

confidence: 99%

ATP-dependent chromatin remodeling during mammalian development

2016

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Precise gene expression ensures proper stem and progenitor cell differentiation, lineage commitment and organogenesis during mammalian development. ATP-dependent chromatin-remodeling complexes utilize the energy from ATP hydrolysis to reorganize chromatin and, hence, regulate gene expression. These complexes contain diverse subunits that together provide a multitude of functions, from early embryogenesis through cell differentiation and development into various adult tissues. Here, we review the functions of chromatin remodelers and their different subunits during mammalian development. We discuss the mechanisms by which chromatin remodelers function and highlight their specificities during mammalian cell differentiation and organogenesis.

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“…In particular, SMARCB1 is required in the SWI/SNF chromatin remodeling complex for controlling the differentiation potential of MRT cells (14)(15)(16). Furthermore, mounting evidence supports a role for SMARCB1 and functional chromatin remodeling complexes in cellular lineage commitment and differentiation, including myogenic (15,17), adipogenic (18), and erythropoietic (19) differentiation pathways.…”

Section: Introductionmentioning

confidence: 99%

Low-Dose Histone Deacetylase Inhibitor Treatment Leads to Tumor Growth Arrest and Multi-Lineage Differentiation of Malignant Rhabdoid Tumors

Muscat

Popovski

Jayasekara

et al. 2016

Clinical Cancer Research

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Purpose: Malignant rhabdoid tumor (MRT) and atypical teratoid rhabdoid tumors (ATRT) are rare aggressive undifferentiated tumors primarily affecting the kidney and CNS of infants and young children. MRT are almost exclusively characterized by homozygous deletion or inactivation of the chromatin remodeling gene SMARCB1. SMARCB1 protein loss leads to direct impairment of chromatin remodeling and we have previously reported a role for this protein in histone acetylation. This provided the rationale for investigating the therapeutic potential of histone deactylase inhibitors (HDACi) in MRT.Experimental Design: Whereas previously HDACis have been used at doses and schedules that induce cytotoxicity, in the current studies we have tested the hypothesis, both in vitro and in vivo, that sustained treatment of human MRT with lowdose HDACi can lead to sustained cell growth arrest and differentiation.

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The chromatin-remodeling enzyme BRG1 plays an essential role in primitive erythropoiesis and vascular development

Cited by 117 publications

References 41 publications

BRG1 promotesCOUP-TFIIexpression and venous specification during embryonic vascular development

BRG1 promotesCOUP-TFIIexpression and venous specification during embryonic vascular development

ATP-dependent chromatin remodeling during mammalian development

Low-Dose Histone Deacetylase Inhibitor Treatment Leads to Tumor Growth Arrest and Multi-Lineage Differentiation of Malignant Rhabdoid Tumors

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