Histone deacetylase (HDAC) 1 and 2 are essential for accurate cell division and the pluripotency of embryonic stem cells

Jamaladdin, Shereen; Kelly, Richard; O’Regan, Laura; Dovey, Oliver M.; Hodson, Grace E.; Millard, Christopher; Portolano, Nicola; Fry, Andrew M.; Schwabe, John W. R.; Cowley, Shaun M.

doi:10.1073/pnas.1321330111

Cited by 138 publications

(158 citation statements)

References 42 publications

(59 reference statements)

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“…ChIP-qPCR at the same six ESC and six EpiC enhancers done for BRG1 validated these results and extended them to HDAC2, which is commonly found in a complex with HDAC1 (Lai and Wade, 2011;Jamaladdin et al, 2014) (Figures S5D and S5E). Consistent with a role for FOXD3 in recruiting as well as maintaining HDAC1 at the FOXD3-bound enhancer sites, HDAC1 was not found at the EpiC enhancers prior to FOXD3 binding (compare Figure 6K to 6L).…”

Section: Foxd3 Also Recruits and Maintains Hdac1/2 At Enhancerssupporting

confidence: 58%

“…IP of FOXD3 showed that FOXD3 protein interacts with HDAC1/2, but not HDAC3, in both ESCs and EpiCs cells ( Figure 6G). As was the case with Brg1, evaluation of published expression data for HDAC1/2 double KO ESCs showed significant overlap in expression changes with Foxd3 KO cells, which was further enriched when considering only genes neighboring the FOXD3 enhancers ( Figure 6H) (Jamaladdin et al, 2014).…”

Section: Foxd3 Also Recruits and Maintains Hdac1/2 At Enhancersmentioning

confidence: 79%

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FOXD3 Regulates Pluripotent Stem Cell Potential by Simultaneously Initiating and Repressing Enhancer Activity

Krishnakumar¹,

Chen²,

Pantovich³

et al. 2018

Cell Stem Cell

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SUMMARYEarly development is governed by the ability of pluripotent cells to retain the full range of developmental potential and respond accurately to developmental cues. This property is achieved in large part by the temporal and contextual regulation of gene expression by enhancers. Here, we evaluated regulation of enhancer activity during differentiation of embryonic stem to epiblast cells and uncovered the forkhead transcription factor FOXD3 as a major regulator of the developmental potential of both pluripo-tent states. FOXD3 bound to distinct sites in the two cell types priming enhancers through a dual-functional mechanism. It recruited the SWI/SNF chromatin remodeling complex ATPase BRG1 to promote nucleosome removal while concurrently inhibiting maximal activation of the same enhancers by recruiting histone deacetylases1/2. Thus, FOXD3 prepares cognate genes for future maximal expression by establishing and simultaneously repressing enhancer activity. Through switching of target sites, FOXD3 modulates the developmental potential of pluripotent cells as they differentiate.

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Section: Foxd3 Also Recruits and Maintains Hdac1/2 At Enhancerssupporting

confidence: 58%

Section: Foxd3 Also Recruits and Maintains Hdac1/2 At Enhancersmentioning

confidence: 79%

FOXD3 Regulates Pluripotent Stem Cell Potential by Simultaneously Initiating and Repressing Enhancer Activity

Krishnakumar¹,

Chen²,

Pantovich³

et al. 2018

Cell Stem Cell

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“…HDAC1 overexpression has been reported to be positively associated with cell division, differentiation and tumorigenesis (28)(29)(30). Loss of HDAC1 resulted in a 60% reduction in total HDAC activity and a loss of stem cell viability (28). Consistently, total HDAC activity was also elevated in A549-CHI-R and A549 HDAC1-overexpressed cells.…”

Section: Discussionmentioning

confidence: 82%

“…HDAC1 belongs to class I HDACs, which are the most closely associated with malignant phenotypes (27). HDAC1 overexpression has been reported to be positively associated with cell division, differentiation and tumorigenesis (28)(29)(30). Loss of HDAC1 resulted in a 60% reduction in total HDAC activity and a loss of stem cell viability (28).…”

Section: Discussionmentioning

confidence: 99%

Molecular, biological characterization and drug sensitivity of chidamide‑resistant non‑small cell lung cancer cells

Luo

Zhu

et al. 2017

Oncol Lett

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Abstract. Chidamide, a histone deacetylase (HDAC) inhibitor, has been applied in clinical trials for various types of hematological and solid tumors. Although acquired resistance is common in chemotherapy, the mechanism of resistance to chidamide is poorly characterized. The goal of the present study was to explore, in detail, the mechanism for the induced resistance to chidamide, and investigate a potential cross-resistance to other chemotherapeutic drugs. A549 cells were exposed to gradually increasing chidamide concentrations to establish a chidamide-resistant non-small cell lung cancer cell line (A549-CHI-R). The IC 50 for chidamide, the proliferation inhibition rate, the total HDAC activity and the HDAC protein level were determined by an MTT assay, colony formation, a fluorometric HDAC activity assay and western blotting, respectively. Overexpression of the HDAC1 gene and HDAC1 gene-knockdown were achieved via plasmid transfection. A549-CHI-R cells demonstrated increased resistance to chidamide (8.6-fold). HDAC1 protein degradation was inhibited and HDAC activity was significantly higher in the A549-CHI-R cells relative to the parental A549 cells. A549-CHI-R cells demonstrated cross-resistance to paclitaxel, vinorelbine and gemcitabine, but not to cisplatin (CDDP) or 5-fluorouracil (5-FU). These results indicated that HDAC1 may be associated with resistance to chidamide, and HDAC1 may therefore be a predictive marker for chidamide sensitivity in cancer. In addition, A549-CHI-R cells remained sensitive to 5-FU and CDDP, indicating a potential strategy for cancer therapy.

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“…Intriguingly, recent studies have suggested that glycans can contribute to epigenetic gene regulation as modulators. For example, a Bcarbohydrate-like^ molecule, inositol tetraphosphate (IP4; inositol 1, 3, 4, 5– tetrakisphosphate) acts as a stimulator to the activity of class I HDACs (HDAC1/2/3) [16–18]. Additionally, OGlcNAcylation has been reported to regulate localization, activity, and stability of many transcription factors, as well as their interactions with other proteins and DNA [19, 20].…”

Section: Introductionmentioning

confidence: 99%

Epigenetic regulation of ganglioside expression in neural stem cells and neuronal cells

Itokazu

Tsai

2016

Glycoconj J

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The structural diversity and localization of cell surface glycosphingolipids (GSLs), including gangliosides, in glycolipid-enriched microdomains (GEMs, also known as lipid rafts) render them ideally suited to play important roles in mediating intercellular recognition, interactions, adhesion, receptor function, and signaling. Gangliosides, sialic acid-containing GSLs, are most abundant in the nerve tissues. The quantity and expression pattern of gangliosides in brain change drastically throughout development and these changes are mainly regulated through stage-specific expression of glycosyltransferase genes. We previously demonstrated for the first time that efficient histone acetylation of the glycosyltransferase genes in mouse brain contributes to the developmental alteration of ganglioside expression. We further demonstrated that acetylation of histones H3 and H4 on the N-acetylgalactosaminyltransferase I (GalNAcT, GA2/GM2/GD2/GT2-synthase; B4galnt1) gene promoter resulted in recruitment of trans-activation factors. In addition, we showed that epigenetic activation of the GalNAcT gene was detected and accompanied by an apparent induction of neuronal differentiation of neural stem cells (NSCs) responding to an exogenous supplement of ganglioside GM1. Most recently, we found that nuclear GM1 binds with acetylated histones on the promoters of the GalNAcT as well as on the NeuroD1 genes in differentiated neurons. Here, we will introduce epigenetic regulation of ganglioside synthase genes in neural development and neuronal differentiation of NSCs.

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Histone deacetylase (HDAC) 1 and 2 are essential for accurate cell division and the pluripotency of embryonic stem cells

Cited by 138 publications

References 42 publications

FOXD3 Regulates Pluripotent Stem Cell Potential by Simultaneously Initiating and Repressing Enhancer Activity

FOXD3 Regulates Pluripotent Stem Cell Potential by Simultaneously Initiating and Repressing Enhancer Activity

Molecular, biological characterization and drug sensitivity of chidamide‑resistant non‑small cell lung cancer cells

Epigenetic regulation of ganglioside expression in neural stem cells and neuronal cells

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