EZH2-Mediated H3K27me3 Targets Transcriptional Circuits of Neuronal Differentiation

Buontempo, Serena; Laise, Pasquale; Hughes, James M.; Trattaro, Sebastiano; Das, Vivek; Rencurel, Chantal; Testa, Giuseppe

doi:10.3389/fnins.2022.814144

Cited by 9 publications

(11 citation statements)

References 89 publications

(121 reference statements)

Supporting

Mentioning

Contrasting

Order By: Relevance

“…Moreover, co-immunoprecipitation of AR and KDM6A has been reported in prostate cancer cells (expressing the oncogenic TMPRSS2:ERG gene fusion) [209] and AR has been demonstrated to decrease expression of KDM6B [210]. Additionally, the Polycomb repressor complex 2 (PRC2) adds H3K27me3 repressive marks [211] and its catalytic subunit (EZH2 [212]) and required subunit for H3K27me3 binding (EED [213]) directly regulate AR binding to hormone response elements [214]. Lastly, querying the protein interaction network between AR, KDM6A, EZH2 and EED as predicted via STRING (a database of known and predicted protein-protein interactions) returns statistically significant protein-protein interaction enrichment in both humans (p = 0.0001) and mice (p = 0.005) [215].…”

Section: Discussionmentioning

confidence: 99%

Gonadal Sex and Sex-Chromosome Complement Interact to Affect Ethanol Consumption in Adolescent Four Core Genotypes Mice

Aarde

Bagley

Jentsch

2022

Preprint

View full text Add to dashboard Cite

Background: Sex differences in ethanol consumption have been reported in both humans and laboratory rodents, but the independent/dependent contributions of genetic and hormonal sex‑biasing mechanisms to these phenotypes have not yet been fully explored. Methods: To examine the contributions of sex-chromosome complement (SCC) and gonadal sex (GS) to ethanol consumption, we studied adolescent (28-32 days old) four core genotypes (FCG) mice (C57BL/6J background; FCG model allows for independent assortment of GS and SCC) using a modified drinking-in-the-dark (DID) procedure. Mice were offered concurrent access to 20%, 10% and 0% ethanol (in water) in four daily 2-hour sessions. Consumption at the level of individual bouts was recorded. Results: Although all four genotype groups preferred the 20% ethanol over 10% and 0%, and showed similar consumption of the 10% and 0% solutions, the group rankings for consumption of the 20% ethanol solution were XX+testes > XY+testes > XY+ovaries > XX+ovaries. Thus, an interaction was observed between SCC and GS for which the simple effect of SCC was greatest in mice with ovaries (XY > XX) and the simple effect of GS was greatest in XX mice (testes > ovaries). Moreover, these effects varied in magnitude across and within drinking sessions. The behavioral microstructure of ethanol consumption (i.e., parameterization of within-session discriminable drinking bouts) support the validity of our 3-bottle modification of the DID procedure as a model of binge-like consumption as: (1) the consumption rate of the 20% ethanol solution was ~80 g EtOH/kg/h within a bout (~12 s/bout, ~3 bouts/session), (2) most of this ethanol consumption was completed in a single bout and (3) within-session ethanol consumption was greater earlier than later, indicating "front loading." Conclusions: These results indicate that SCC and GS interact on ethanol consumption in adolescent FCG mice on a C57BL/6J background to affect binge-like consumption from the very initiation of access and that these effects are dynamic as they varied both across and within sessions.

show abstract

Section: Discussionmentioning

confidence: 99%

Gonadal Sex and Sex-Chromosome Complement Interact to Affect Ethanol Consumption in Adolescent Four Core Genotypes Mice

Aarde

Bagley

Jentsch

2022

Preprint

View full text Add to dashboard Cite

show abstract

“…EED ablation also resulted in functional deficits manifested in the altered electrophysiological properties of the neurons, abnormal production of cell-specific metabolites, and pathological behavioral phenotypes in mice [ 153 ]. In agreement with this, conditional EZH2 inactivation via Cre -inducible deletion of the SET domain in glutamatergic neurons in vitro led to their altered differentiation trajectory and the switch towards a transcriptomic signature associated with GABAergic neurons [ 132 ]. The enhancement in GABAergic signature and the overproduction of interneurons following EZH2 ablation was also shown in mouse cerebellum [ 155 ], further implicating PRC2 in the establishment and maintenance of neuronal identity, as well as the balance between the different neuronal populations.…”

Section: Introductionmentioning

confidence: 85%

“…PRC2 is involved in transcriptional silencing through its methyltransferase (HMT) activity, catalyzing the mono-, di-, and tri-methylation of H3K27 [ 130 , 131 ]. It has many roles specifically within the central nervous system, including effects on maturation [ 132 ], proliferation [ 133 ], and the identity of neural stem cells [ 134 ], migration and maturation of neurons [ 135 ], and gliogenesis [ 136 , 137 ]. The proper function of PRC2 is required for the silencing of specific genes to allow the transcription of other genes that mediate alternative cellular processes.…”

Section: Introductionmentioning

confidence: 99%

“…EZH2-KO results in the reduction of neural progenitor proliferation Liu et al [ 166 ] Appropriate neuronal orientation and cortical radial migration EZH2 inhibition results in abnormal neuronal orientation reduced neuronal numbers at the cortical plate and ectopic expression of Reelin Zhao et al [ 135 ] EZH2-mediated repression of Netrin1 is necessary for the appropriate migration of pontine neurons in the cortico-ponto-cerebellar pathway in mice. EZH2-KO results in ectopic Netrin1 induction and aberrant neuronal migration Di Meglio et al [ 156 ] Maintenance of neuronal identity Deletion of EED disrupts the acquisition and maintenance of neuronal identity and functionality in differentiated dopaminergic and serotonergic neurons Toskas et al [ 153 ] Conditional knock-out of EZH2 results in reduced proliferation of granule precursor cells, decrease in the Purkinje cell population and increase in GABAergic interneurons in the mouse cerebellum Feng et al [ 155 ] Conditional KO of EZH2 results in loss of H3K27me3 marks in differentiating neurons and causes changes to molecular networks that govern glutamatergic neuron differentiation, leading to a disruption in the balance of inhibitory/excitatory neurons during the development Buontempo et al [ 132 ] Combined EZH1 and EZH2 KO leads to a loss of H3K27me3 marks in MSNs in the striatum, down-regulation of lineage-specific and function-specific MSN genes, and upregulation of the death-promoting genes Von Schimmelmann et al [ 154 ] Glial cell development and fate determination Pharmacological inhibition of EZH2 leads to increased expression of Olig1 and Olig2. Increased depositions of H3K27me3 marks are detected in the genomic loci of Olig1 and Olig2 in HMGN-KO ESCs Deng et al [ 124 ] KO of EZH2 or EED do not affect the generation of OPC but inhibit their differentiation into mature, myelinating oligodendrocytes.…”

Section: Introductionmentioning

confidence: 99%

“…The underproduction of GABAergic neurons and their abnormal migration was also demonstrated in an in vitro model derived from DS iPSCs and attributed to the increased levels of p21-activated kinase 1 (PAK1) [ 242 ], a binding target for SUZ12 [ 68 ]. Moreover, the commitment and lineage development of inhibitory neurons are PRC2-dependent [ 132 , 243 ] and while OLIG2 is triplicated in DS, it is also known to be highly regulated by HMGN1 [ 121 ], suggesting that despite the above discrepancy between the studies, there is a consistency in reported deficits in the interneuron motility and the disbalance between the excitatory and inhibitory neurons that can be potentially caused by the gene dosage of HMGN1 and subsequent dysregulation of PRC2 targets.…”

Section: Introductionmentioning

confidence: 99%

See 2 more Smart Citations

Shaking up the silence: consequences of HMGN1 antagonizing PRC2 in the Down syndrome brain

Farley

Grishok

Zeldich

2022

Epigenetics & Chromatin

View full text Add to dashboard Cite

Intellectual disability is a well-known hallmark of Down Syndrome (DS) that results from the triplication of the critical region of human chromosome 21 (HSA21). Major studies were conducted in recent years to gain an understanding about the contribution of individual triplicated genes to DS-related brain pathology. Global transcriptomic alterations and widespread changes in the establishment of neural lineages, as well as their differentiation and functional maturity, suggest genome-wide chromatin organization alterations in trisomy. High Mobility Group Nucleosome Binding Domain 1 (HMGN1), expressed from HSA21, is a chromatin remodeling protein that facilitates chromatin decompaction and is associated with acetylated lysine 27 on histone H3 (H3K27ac), a mark correlated with active transcription. Recent studies causatively linked overexpression of HMGN1 in trisomy and the development of DS-associated B cell acute lymphoblastic leukemia (B-ALL). HMGN1 has been shown to antagonize the activity of the Polycomb Repressive Complex 2 (PRC2) and prevent the deposition of histone H3 lysine 27 trimethylation mark (H3K27me3), which is associated with transcriptional repression and gene silencing. However, the possible ramifications of the increased levels of HMGN1 through the derepression of PRC2 target genes on brain cell pathology have not gained attention. In this review, we discuss the functional significance of HMGN1 in brain development and summarize accumulating reports about the essential role of PRC2 in the development of the neural system. Mechanistic understanding of how overexpression of HMGN1 may contribute to aberrant brain cell phenotypes in DS, such as altered proliferation of neural progenitors, abnormal cortical architecture, diminished myelination, neurodegeneration, and Alzheimer’s disease-related pathology in trisomy 21, will facilitate the development of DS therapeutic approaches targeting chromatin.

show abstract

Role of NAD+ and FAD in Ischemic Stroke Pathophysiology: An Epigenetic Nexus and Expanding Therapeutic Repertoire

Narne

Babu

2022

Cell Mol Neurobiol

View full text Add to dashboard Cite

EZH2-Mediated H3K27me3 Targets Transcriptional Circuits of Neuronal Differentiation

Cited by 9 publications

References 89 publications

Gonadal Sex and Sex-Chromosome Complement Interact to Affect Ethanol Consumption in Adolescent Four Core Genotypes Mice

Gonadal Sex and Sex-Chromosome Complement Interact to Affect Ethanol Consumption in Adolescent Four Core Genotypes Mice

Shaking up the silence: consequences of HMGN1 antagonizing PRC2 in the Down syndrome brain

Role of NAD+ and FAD in Ischemic Stroke Pathophysiology: An Epigenetic Nexus and Expanding Therapeutic Repertoire

Contact Info

Product

Resources

About