Molecular Oncology Group, Institute of Pathology, Medical Faculty of the RWTH Aachen University, Aachen, Germany.
Oncogene. 2010 Aug 26;29(34):4814-25. doi: 10.1038/onc.2010.229. Epub 2010 Jun 14.
Synemin (SYNM) is a type IV intermediate filament that has recently been shown to interact with the LIM domain protein zyxin, thereby possibly modulating cell adhesion and cell motility. Owing to this multiplicity of potential functions relevant to cancer development, we initiated a study to decipher SYNM expression and regulation in benign human breast tissue and breast cancer. Dot blot array analysis showed significant SYNM mRNA downregulation in 86% (n=100, P<0.001) of breast cancers compared with their normal tissue counterparts, a result that was confirmed by real-time PCR analysis (n=36, P<0.0001). Immunohistochemistry analysis showed abundant SYNM protein expression in healthy myoepithelial breast cells, whereas SYNM expression loss was evident in 57% (n=37, P<0.001) of breast cancer specimens. Next, we analyzed methylation of the SYNM promoter to clarify whether the SYNM gene can be silenced by epigenetic means. Indeed, methylation-specific PCR analysis showed tumor-specific SYNM promoter methylation in 27% (n=195) of breast cancers. As expected, SYNM promoter methylation was tightly associated (P<0.0001) with SYNM expression loss. In-depth analysis of the SYNM promoter by pyrosequencing showed extensive CpG methylation of DNA elements supposed to regulate gene transcription. Demethylating treatment of SYNM methylated breast cancer cell lines with 5-aza-2-deoxycytidine clearly reestablished the SYNM expression. Statistical analysis of the patient cohort showed a close association between SYNM promoter methylation and unfavorable recurrence-free survival (hazard ratio=2.941, P=0.0282). Furthermore, SYNM methylation positively correlated with lymph node metastases (P=0.0177) and advanced tumor grade (P=0.0275), suggesting that SYNM methylation is associated with aggressive forms of breast cancer. This is the first study on the epigenetic regulation of the SYNM gene in a cancer entity. We provide first hints that SYNM could represent a novel putative breast tumor suppressor gene that is prone to epigenetic silencing. SYNM promoter methylation may become a useful predictive biomarker to stratify breast cancer patients' risk for tumor relapse.
神经束蛋白(SYNM)是一种 IV 型中间丝,最近研究表明其与 LIM 结构域蛋白 zyxin 相互作用,从而可能调节细胞黏附和细胞运动。由于这种多功能性可能与癌症的发生有关,我们开始研究良性人乳腺组织和乳腺癌中 SYNM 的表达和调节。点印迹分析显示,与正常组织相比,86%(n=100,P<0.001)的乳腺癌中 SYNM mRNA 表达显著下调,实时 PCR 分析(n=36,P<0.0001)证实了这一点。免疫组化分析显示,健康的乳腺肌上皮细胞中 SYNM 蛋白表达丰富,而 57%(n=37,P<0.001)的乳腺癌标本中 SYNM 表达缺失。接下来,我们分析了 SYNM 启动子的甲基化,以阐明 SYNM 基因是否可以通过表观遗传机制沉默。事实上,甲基化特异性 PCR 分析显示,27%(n=195)的乳腺癌中存在肿瘤特异性 SYNM 启动子甲基化。正如预期的那样,SYNM 启动子甲基化与 SYNM 表达缺失密切相关(P<0.0001)。焦磷酸测序对 SYNM 启动子的深入分析显示,DNA 元件的广泛 CpG 甲基化可能调节基因转录。用 5-氮杂-2-脱氧胞苷对 SYNM 甲基化的乳腺癌细胞系进行去甲基化处理,明显重新建立了 SYNM 的表达。对患者队列的统计分析表明,SYNM 启动子甲基化与不良无复发生存率密切相关(风险比=2.941,P=0.0282)。此外,SYNM 甲基化与淋巴结转移(P=0.0177)和高级别肿瘤(P=0.0275)呈正相关,表明 SYNM 甲基化与侵袭性乳腺癌有关。这是首次在癌症实体中研究 SYNM 基因的表观遗传调控。我们首次提示 SYNM 可能代表一种新的潜在的乳腺癌肿瘤抑制基因,易发生表观遗传沉默。SYNM 启动子甲基化可能成为一种有用的预测生物标志物,用于分层乳腺癌患者的肿瘤复发风险。
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