Inhibition of Euchromatic Histone Lysine Methyltransferase 2 (EHMT2) Suppresses the Proliferation and Invasion of Cervical Cancer Cells

Chen, Guoqiang; Yu, Xiaqing; Zhang, Min; Zheng, Ai; Wang, Zhennan; Zuo, Yufang; Liang, Qiong; Jiang, Danxian; Chang, Yaqing; Zhao, Liang; Jiang, Liyuan; Li, Dan; Liao, Sihai

doi:10.1159/000502072

Cited by 5 publications

(5 citation statements)

References 27 publications

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“…These epigenetic modifications, which result in altered chromatin structure and gene expression were reported in different types of cancers [ 108 ] ( Figure 3 ). G9a was overexpressed in breast, gastric, ovarian, cervical, endometrial, prostate, lung, colorectal, liver, urinary bladder, and brain cancers, as well as in hematological malignancies, melanoma, and cholangiocarcinoma, leading to aberrant H3K9 methylation [ 109 , 110 , 111 , 112 , 113 , 114 , 115 , 116 , 117 , 118 , 119 , 120 , 121 , 122 ]. One of the main reasons for this increase in G9a expression and H3K9 methylation is hypoxia [ 103 ].…”

Section: G9a In Cancermentioning

confidence: 99%

“…In cervical cancer, G9a induces the expression of angiogenic factors including angiogenin, interleukin-8, and C-X-C motif chemokine ligand-16, prompting angiogenesis and cancer cell invasion, and decreasing patient survival [ 142 ]. Interestingly, depletion of G9a decreased the expression of oncogenic proteins such as Bcl-2, Mcl-1, and Survivin, and increased the expression of E-cadherin inhibiting cell adhesion and invasion [ 112 ].…”

Section: G9a In Cancermentioning

confidence: 99%

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Structure, Activity, and Function of the Protein Lysine Methyltransferase G9a

Poulard

Noureddine

Pruvost

et al. 2021

Life

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G9a is a lysine methyltransferase catalyzing the majority of histone H3 mono- and dimethylation at Lys-9 (H3K9), responsible for transcriptional repression events in euchromatin. G9a has been shown to methylate various lysine residues of non-histone proteins and acts as a coactivator for several transcription factors. This review will provide an overview of the structural features of G9a and its paralog called G9a-like protein (GLP), explore the biochemical features of G9a, and describe its post-translational modifications and the specific inhibitors available to target its catalytic activity. Aside from its role on histone substrates, the review will highlight some non-histone targets of G9a, in order gain insight into their role in specific cellular mechanisms. Indeed, G9a was largely described to be involved in embryonic development, hypoxia, and DNA repair. Finally, the involvement of G9a in cancer biology will be presented.

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Section: G9a In Cancermentioning

confidence: 99%

Section: G9a In Cancermentioning

confidence: 99%

Structure, Activity, and Function of the Protein Lysine Methyltransferase G9a

Poulard

Noureddine

Pruvost

et al. 2021

Life

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“…An array-CGH was performed. The Agilent Bench Lab CNV Version 5.1 180 K array-CGH showed a de novo deletion on chromosome 6p25.3 of ~403 kb (Figure 2) and a maternally inherited duplication in Xq27.2 of ~316 kb (arr [GRCh37] 6p25.3(1727928_2131157) x1 dn, Xq27.2(140693307_141009050) x3 mat, in accordance with the ISCN 2020 nomenclature [18]. No (likely) pathogenic variants were identified in the NGS gene panel.…”

Section: Molecular and Cytogenetic Studiesmentioning

confidence: 60%

GMDS Intragenic Deletions Associate with Congenital Heart Disease including Ebstein Anomaly

et al. 2023

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Ebstein anomaly is a rare heterogeneous congenital heart defect (CHD) with a largely unknown etiology. We present a 6-year-old girl with Ebstein anomaly, atrial septum defect, hypoplastic right ventricle, and persistent left superior vena cava who has a de novo intragenic ~403 kb deletion of the GDP-mannose 4,6-dehydratase (GMDS) gene. GMDS is located on chromosome 6p25.3 and encodes the rate limiting enzyme in GDP-fucose synthesis, which is used to fucosylate many proteins, including Notch1, which plays a critical role during mammalian cardiac development. The GMDS locus has sporadically been associated with Ebstein anomaly (large deletion) and tetralogy of Fallot (small deletion). Given its function and the association with CHD, we hypothesized that loss-of-function of, or alterations in, GMDS could play a role in the development of Ebstein anomaly. We collected a further 134 cases with Ebstein anomaly and screened them for genomic aberrations of the GMDS locus. No additional GMDS genomic aberrations were identified. In conclusion, we describe a de novo intragenic GMDS deletion associated with Ebstein anomaly. Together with previous reports, this second case suggests that GMDS deletions could be a rare cause for congenital heart disease, in particular Ebstein anomaly.

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“…Human cervical cancer cell lines (CaloGR) exhibit high levels of EHMT2 as compared to cervical epithelial cells. Loss‐of‐function studies indicated a reduction in cell adhesion and invasive capacities through downregulation of E‐cadherin [38]. Pharmacological and genetic inhibition of EHMT2 impeded angiogenesis, invasion and migration both in vitro and in vivo , with a reduction in the expression of angiogenic genes including CXCL16, IL‐8, VEGF, MMP9, MCP‐1, Pentraxin‐3, GM‐CSF, Serpin E1,TIMP‐1, TIMP‐4 and Thrombospondin‐1 [39].…”

Section: Cancer Metastasismentioning

confidence: 99%

EHMT1/EHMT2 in EMT, cancer stemness and drug resistance: emerging evidence and mechanisms

2022

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Metastasis, therapy failure and tumour recurrence are major clinical challenges in cancer. The interplay between tumour‐initiating cells (TICs) and epithelial–mesenchymal transition (EMT) drives tumour progression and spread. Recent advances have highlighted the involvement of epigenetic deregulation in these processes. The euchromatin histone lysine methyltransferase 1 (EHMT1) and euchromatin histone lysine methyltransferase 2 (EHMT2) that primarily mediate histone 3 lysine 9 di‐methylation (H3K9me2), as well as methylation of non‐histone proteins, are now recognised to be aberrantly expressed in many cancers. Their deregulated expression is associated with EMT, cellular plasticity and therapy resistance. In this review, we summarise evidence of their myriad roles in cancer metastasis, stemness and drug resistance. We discuss cancer‐type specific molecular targets, context‐dependent mechanisms and future directions of research in targeting EHMT1/EHMT2 for the treatment of cancer.

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Inhibition of Euchromatic Histone Lysine Methyltransferase 2 (EHMT2) Suppresses the Proliferation and Invasion of Cervical Cancer Cells

Cited by 5 publications

References 27 publications

Structure, Activity, and Function of the Protein Lysine Methyltransferase G9a

Structure, Activity, and Function of the Protein Lysine Methyltransferase G9a

GMDS Intragenic Deletions Associate with Congenital Heart Disease including Ebstein Anomaly

EHMT1/EHMT2 in EMT, cancer stemness and drug resistance: emerging evidence and mechanisms

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