Department of Oncohematology, Ospedale Pediatrico Bambino Gesù, IRCCS, Roma, Italy.
IRCCS Fondazione Santa Lucia, Roma, Italy.
Oncogene. 2014 Aug 7;33(32):4173-84. doi: 10.1038/onc.2013.471. Epub 2013 Nov 11.
The Polycomb group (PcG) proteins regulate stem cell differentiation via the repression of gene transcription, and their deregulation has been widely implicated in cancer development. The PcG protein Enhancer of Zeste Homolog 2 (EZH2) works as a catalytic subunit of the Polycomb Repressive Complex 2 (PRC2) by methylating lysine 27 on histone H3 (H3K27me3), a hallmark of PRC2-mediated gene repression. In skeletal muscle progenitors, EZH2 prevents an unscheduled differentiation by repressing muscle-specific gene expression and is downregulated during the course of differentiation. In rhabdomyosarcoma (RMS), a pediatric soft-tissue sarcoma thought to arise from myogenic precursors, EZH2 is abnormally expressed and its downregulation in vitro leads to muscle-like differentiation of RMS cells of the embryonal variant. However, the role of EZH2 in the clinically aggressive subgroup of alveolar RMS, characterized by the expression of PAX3-FOXO1 oncoprotein, remains unknown. We show here that EZH2 depletion in these cells leads to programmed cell death. Transcriptional derepression of F-box protein 32 (FBXO32) (Atrogin1/MAFbx), a gene associated with muscle homeostasis, was evidenced in PAX3-FOXO1 RMS cells silenced for EZH2. This phenomenon was associated with reduced EZH2 occupancy and H3K27me3 levels at the FBXO32 promoter. Simultaneous knockdown of FBXO32 and EZH2 in PAX3-FOXO1 RMS cells impaired the pro-apoptotic response, whereas the overexpression of FBXO32 facilitated programmed cell death in EZH2-depleted cells. Pharmacological inhibition of EZH2 by either 3-Deazaneplanocin A or a catalytic EZH2 inhibitor mirrored the phenotypic and molecular effects of EZH2 knockdown in vitro and prevented tumor growth in vivo. Collectively, these results indicate that EZH2 is a key factor in the proliferation and survival of PAX3-FOXO1 alveolar RMS cells working, at least in part, by repressing FBXO32. They also suggest that the reducing activity of EZH2 could represent a novel adjuvant strategy to eradicate high-risk PAX3-FOXO1 alveolar RMS.
多梳抑制复合物(PcG)蛋白通过抑制基因转录来调节干细胞分化,其失调已广泛涉及癌症的发生。PcG 蛋白 Enhancer of Zeste Homolog 2(EZH2)作为 Polycomb 抑制复合物 2(PRC2)的催化亚基发挥作用,通过将组蛋白 H3 赖氨酸 27 甲基化(H3K27me3)来抑制基因转录,这是 PRC2 介导的基因抑制的标志。在骨骼肌祖细胞中,EZH2 通过抑制肌肉特异性基因表达来防止非计划分化,并在分化过程中下调。在横纹肌肉瘤(RMS)中,一种被认为起源于成肌前体的小儿软组织肉瘤,EZH2 异常表达,其在体外的下调导致胚胎变异 RMS 细胞的肌肉样分化。然而,EZH2 在具有 PAX3-FOXO1 癌蛋白表达的临床侵袭性肺泡 RMS 的亚组中的作用仍然未知。我们在这里表明,这些细胞中 EZH2 的耗竭导致程序性细胞死亡。转录去抑制 F-box 蛋白 32(FBXO32)(Atrogin1/MAFbx),一种与肌肉动态平衡相关的基因,在 EZH2 沉默的 PAX3-FOXO1 RMS 细胞中被证明。这种现象与 FBXO32 启动子处的 EZH2 占据减少和 H3K27me3 水平降低有关。在 PAX3-FOXO1 RMS 细胞中同时敲低 FBXO32 和 EZH2 会损害促凋亡反应,而 FBXO32 的过表达则促进 EZH2 耗竭细胞中的程序性细胞死亡。通过 3-去氮杂胞苷 A 或催化 EZH2 抑制剂抑制 EZH2 的药理学抑制在体外模拟了 EZH2 敲低的表型和分子效应,并防止了体内肿瘤生长。总之,这些结果表明 EZH2 是 PAX3-FOXO1 肺泡 RMS 细胞增殖和存活的关键因素,至少部分通过抑制 FBXO32 发挥作用。它们还表明,降低 EZH2 的活性可能代表一种新的辅助策略来根除高危 PAX3-FOXO1 肺泡 RMS。
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