USP44 Overexpression Drives a MYC-Like Gene Expression Program in Neuroblastoma through Epigenetic Reprogramming.

IF 4.1 2区 医学 Q2 CELL BIOLOGY Molecular Cancer Research Pub Date : 2024-09-04 DOI:10.1158/1541-7786.MCR-23-0454
Thomas L Ekstrom, Sajjad Hussain, Tibor Bedekovics, Asma Ali, Lucia Paolini, Hina Mahmood, Raya M Rosok, Jan Koster, Steven A Johnsen, Paul J Galardy
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Abstract

Neuroblastoma is an embryonic cancer that contributes disproportionately to death in young children. Sequencing data have uncovered few recurrently mutated genes in this cancer, although epigenetic pathways have been implicated in disease pathogenesis. We used an expression-based computational screen that examined the impact of deubiquitinating enzymes on patient survival to identify potential new targets. We identified the histone H2B deubiquitinating enzyme USP44 as the enzyme with the greatest impact on survival in patients with neuroblastoma. High levels of USP44 significantly correlate with metastatic disease, unfavorable histology, advanced patient age, and MYCN amplification. The subset of patients with tumors expressing high levels of USP44 had significantly worse survival, including those with tumors lacking MYCN amplification. We showed experimentally that USP44 regulates neuroblastoma cell proliferation, migration, invasion, and neuronal development. Depletion of the histone H2B ubiquitin ligase subunit RNF20 resulted in similar findings, strongly implicating this histone mark as the target of USP44 activity in this disease. Integration of transcriptome and epigenome in analyses demonstrates a distinct set of genes that are regulated by USP44, including those in Hallmark MYC target genes in both murine embryonic fibroblasts and the SH-SY5Y neuroblastoma cell line. We conclude that USP44 is a novel epigenetic regulator that promotes aggressive features and may be a novel target in neuroblastoma. Implications: This study identifies a new genetic marker of aggressive neuroblastoma and identifies the mechanisms by which its overactivity contributes to the pathophysiology of this disease.

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USP44 过表达通过表观遗传重编程驱动神经母细胞瘤中的 MYC 类基因表达程序。
神经母细胞瘤是一种胚胎癌症,导致幼儿死亡的比例极高。尽管表观遗传途径与疾病的发病机制有关,但测序数据发现这种癌症中很少有重复突变的基因。我们利用基于表达的计算筛选,研究了去泛素化酶对患者生存的影响,以确定潜在的新靶点。我们发现组蛋白H2B去泛素化酶USP44是对神经母细胞瘤患者生存影响最大的酶。USP44的高水平与转移性疾病、不利组织学、高龄患者和MYCN扩增密切相关。表达高水平 USP44 的肿瘤患者生存率明显较低,包括那些没有 MYCN 扩增的肿瘤患者。我们的实验表明,USP44 可调节神经母细胞瘤细胞的增殖、迁移、侵袭和神经元发育。组蛋白 H2B 泛素连接酶亚基 RNF20 的缺失也导致了类似的结果,这有力地证明了该组蛋白标记是 USP44 在该疾病中的活性靶标。整合转录组和表观基因组的分析表明,有一组不同的基因受到 USP44 的调控,包括小鼠胚胎成纤维细胞和 SH-SY5Y 神经母细胞瘤细胞系中的 Hallmark MYC 靶基因。我们得出结论:USP44 是一种新型的表观遗传调控因子,可促进侵袭性特征,可能是神经母细胞瘤的新型靶点。意义:这项研究确定了侵袭性神经母细胞瘤的一个新的遗传标记,并确定了其过度活动导致这种疾病的病理生理学的机制。
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来源期刊
Molecular Cancer Research
Molecular Cancer Research 医学-细胞生物学
CiteScore
9.90
自引率
0.00%
发文量
280
审稿时长
4-8 weeks
期刊介绍: Molecular Cancer Research publishes articles describing novel basic cancer research discoveries of broad interest to the field. Studies must be of demonstrated significance, and the journal prioritizes analyses performed at the molecular and cellular level that reveal novel mechanistic insight into pathways and processes linked to cancer risk, development, and/or progression. Areas of emphasis include all cancer-associated pathways (including cell-cycle regulation; cell death; chromatin regulation; DNA damage and repair; gene and RNA regulation; genomics; oncogenes and tumor suppressors; signal transduction; and tumor microenvironment), in addition to studies describing new molecular mechanisms and interactions that support cancer phenotypes. For full consideration, primary research submissions must provide significant novel insight into existing pathway functions or address new hypotheses associated with cancer-relevant biologic questions.
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