INSERM U954, Faculty of Medicine, Université de Lorraine, Vandoeuvre-lès-Nancy, France.
Department of Pathology, CHRU, Nancy, France.
J Pathol. 2017 Aug;242(4):421-434. doi: 10.1002/path.4916. Epub 2017 Jul 5.
HuR regulates cytoplasmic mRNA stability and translatability, and the HuR expression level has been shown to correlate with poor disease outcome in several cancer types; however, the prognostic value and potential pro-oncogenic properties of HuR in meningioma remain unclear. Thus, in the present study, we analysed 85 meningioma tissue samples to establish the relationship between HuR expression, tumour cell proliferation, and/or patient survival. In addition, we examined the anti-proliferative effects of HuR knockdown in two meningioma cell lines (IOMM-Lee and Ben-Men-1) and conducted transcriptome-wide analyses (IOMM-Lee cells) to elucidate the molecular consequences of HuR knockdown. The results of the present study showed HuR cytoplasmic expression to correlate positively with tumour grade (p = 1.2 × 10 ) and negatively with progression-free and overall survival (p = 0.01) time in human meningioma tissues. In vitro, siHuR-induced HuR knockdown was shown to reduce the growth of both Ben-Men-1 (p = 2 × 10 ) and IOMM-Lee (p = 4 × 10 ) cells. Transcriptome analyses revealed HuR knockdown in IOMM-Lee cells to deregulate the HIF1A signalling pathway (p = 1.5 × 10 ) and to up-regulate the expression of genes essential for the assembly of the cytoplasmic mRNA processing body, global genome nucleotide-excision repair, poly(A)-specific ribonuclease activity, the positive regulation of apoptosis and of cell cycle arrest, and the negative regulation of RNA splicing [p(FDR) < 0.001]. Interestingly, HuR knockdown under hypoxic culture conditions further potentiated the effects of HuR knockdown on cell growth, apoptosis, and HIF1A expression. We thus conclude that cytoplasmic HuR expression is a marker of poor prognosis in meningioma and that HuR is a promising potential therapeutic target for use in tumours refractory to standard therapies. Copyright © 2017 Pathological Society of Great Britain and Ireland. Published by John Wiley & Sons, Ltd.
HuR 调节细胞质 mRNA 的稳定性和翻译能力,HuR 的表达水平已被证明与几种癌症类型的不良预后相关;然而,HuR 在脑膜瘤中的预后价值和潜在致癌特性仍不清楚。因此,在本研究中,我们分析了 85 例脑膜瘤组织样本,以建立 HuR 表达、肿瘤细胞增殖和/或患者生存之间的关系。此外,我们还研究了 HuR 敲低对两种脑膜瘤细胞系(IOMM-Lee 和 Ben-Men-1)的抗增殖作用,并进行了全转录组分析(IOMM-Lee 细胞),以阐明 HuR 敲低的分子后果。本研究结果表明,HuR 细胞质表达与肿瘤分级呈正相关(p = 1.2×10-5),与无进展生存期和总生存期呈负相关(p = 0.01)。在体外,siHuR 诱导的 HuR 敲低可降低 Ben-Men-1(p = 2×10-5)和 IOMM-Lee(p = 4×10-5)细胞的生长。转录组分析显示,IOMM-Lee 细胞中的 HuR 敲低可使 HIF1A 信号通路失调(p = 1.5×10-5),并上调细胞质 mRNA 处理体组装、全基因组核苷酸切除修复、聚(A)特异性核糖核酸酶活性、细胞凋亡和细胞周期阻滞的正调节以及 RNA 剪接的负调节所必需基因的表达(p(FDR)<0.001)。有趣的是,在低氧培养条件下敲低 HuR 进一步增强了 HuR 敲低对细胞生长、凋亡和 HIF1A 表达的影响。因此,我们得出结论,细胞质 HuR 表达是脑膜瘤预后不良的标志物,HuR 是治疗标准治疗耐药肿瘤的有前途的潜在治疗靶点。版权所有©2017 英国和爱尔兰病理学学会。由 John Wiley & Sons,Ltd. 出版。
Zotero 插件