Pawel Nowialis, Julian Tobon, Katarina Lopusna, Jana Opavska, Arshee Badar, Duo Chen, Reem Abdelghany, Gene Pozas, Jacob Fingeret, Emma Noel, Alberto Riva, Hiroshi Fujiwara, Alexander Ishov, Rene Opavsky
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We found that the methylation patterns in PTCLs are deregulated and heterogeneous but share 767 hypo- and 567 hypermethylated differentially methylated regions (DMRs) along with 231 genes up- and 91 genes downregulated in all samples, suggesting a potential association with tumor development. We further identified 39 hypomethylated promoters associated with increased gene expression in the majority of PTCLs. This putative oncogenic signature included the <i>TRIP13</i> (thyroid hormone receptor interactor 13) gene whose genetic and pharmacologic inactivation inhibited the proliferation of T-cell lines by inducing G2-M arrest and apoptosis. Our data thus show that human PTCLs have a significant number of recurrent methylation alterations that may affect the expression of genes critical for proliferation whose targeting might be beneficial in anti-lymphoma treatments.</p>","PeriodicalId":55768,"journal":{"name":"Epigenomes","volume":"8 3","pages":""},"PeriodicalIF":2.5000,"publicationDate":"2024-08-21","publicationTypes":"Journal Article","fieldsOfStudy":null,"isOpenAccess":false,"openAccessPdf":"https://www.ncbi.nlm.nih.gov/pmc/articles/PMC11348144/pdf/","citationCount":"0","resultStr":"{\"title\":\"Genome-Wide Methylation Profiling of Peripheral T-Cell Lymphomas Identifies TRIP13 as a Critical Driver of Tumor Proliferation and Survival.\",\"authors\":\"Pawel Nowialis, Julian Tobon, Katarina Lopusna, Jana Opavska, Arshee Badar, Duo Chen, Reem Abdelghany, Gene Pozas, Jacob Fingeret, Emma Noel, Alberto Riva, Hiroshi Fujiwara, Alexander Ishov, Rene Opavsky\",\"doi\":\"10.3390/epigenomes8030032\",\"DOIUrl\":null,\"url\":null,\"abstract\":\"<p><p>Cytosine methylation contributes to the regulation of gene expression and normal hematopoiesis in mammals. 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引用次数: 0
摘要
胞嘧啶甲基化有助于调节哺乳动物的基因表达和正常造血。它由 DNA 甲基转移酶家族(包括 DNMT1、DNMT3A 和 DNMT3B)催化。外周 T 细胞淋巴瘤(PTCL)是一种侵袭性成熟 T 细胞恶性肿瘤,具有广泛的临床特征,预后不良,其分子病理生物学尚不清楚。为了更好地了解其分子结构并确定参与疾病维持的候选基因,我们对 PTCL 的 DNA 甲基化和基因表达进行了分析。我们发现,PTCL 的甲基化模式是失调和异质性的,但在所有样本中,共有 767 个低甲基化和 567 个高甲基化的差异甲基化区域(DMR),231 个基因上调,91 个基因下调,这表明它们与肿瘤的发展有潜在的关联。我们进一步确定了 39 个低甲基化启动子,它们与大多数 PTCL 中基因表达的增加有关。这种假定的致癌特征包括 TRIP13(甲状腺激素受体互作因子 13)基因,该基因的遗传和药物失活可通过诱导 G2-M 停滞和细胞凋亡来抑制 T 细胞系的增殖。因此,我们的数据表明,人类 PTCL 有大量反复发生的甲基化改变,这些改变可能会影响对增殖至关重要的基因的表达,而针对这些基因的治疗可能对抗淋巴瘤治疗有益。
Genome-Wide Methylation Profiling of Peripheral T-Cell Lymphomas Identifies TRIP13 as a Critical Driver of Tumor Proliferation and Survival.
Cytosine methylation contributes to the regulation of gene expression and normal hematopoiesis in mammals. It is catalyzed by the family of DNA methyltransferases that include DNMT1, DNMT3A, and DNMT3B. Peripheral T-cell lymphomas (PTCLs) represent aggressive mature T-cell malignancies exhibiting a broad spectrum of clinical features with poor prognosis and inadequately understood molecular pathobiology. To better understand the molecular landscape and identify candidate genes involved in disease maintenance, we profiled DNA methylation and gene expression of PTCLs. We found that the methylation patterns in PTCLs are deregulated and heterogeneous but share 767 hypo- and 567 hypermethylated differentially methylated regions (DMRs) along with 231 genes up- and 91 genes downregulated in all samples, suggesting a potential association with tumor development. We further identified 39 hypomethylated promoters associated with increased gene expression in the majority of PTCLs. This putative oncogenic signature included the TRIP13 (thyroid hormone receptor interactor 13) gene whose genetic and pharmacologic inactivation inhibited the proliferation of T-cell lines by inducing G2-M arrest and apoptosis. Our data thus show that human PTCLs have a significant number of recurrent methylation alterations that may affect the expression of genes critical for proliferation whose targeting might be beneficial in anti-lymphoma treatments.