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Comprehensive Analysis of the Expression of Key Genes Related to Hippo Signaling and Their Prognosis Impact in Ovarian Cancer

机译:河马信号传导相关关键基因的表达及其在卵巢癌预后综合分析

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摘要

The Hippo signaling pathway, one of the most conserved in humans, controlling dimensions of organs and tumor growth, is frequently deregulated in several human malignancies, including ovarian cancer (OC). The alteration of Hippo signaling has been reported to contribute to ovarian carcinogenesis and progression. However, the prognostic roles of individual Hippo genes in OC patients remain elusive. Herein we investigated the expression level and prognostic value of key Hippo genes in OC using online databases, followed by a qRT-PCR validation step in an additional patient cohort. Using the GEPIA database, we observed an increased level for TP53 and reduced expression level for LATS1, LATS2, MST1, TAZ, and TEF in tumor tissue versus normal adjacent tissue. Moreover, LATS1, LATS2, TP53, TAZ, and TEF expression levels have prognostic significance correlated with progression-free survival. The qRT-PCR validation step was conducted in an OC patient cohort comprising 29 tumor tissues and 20 normal adjacent tissues, endorsing the expression level for LATS1, LATS2, and TP53, as well as for two of the miRNAs targeting the TP53 gene, revealing miR-25-3p upregulation and miR-181c-5p downregulation. These results display that there are critical prognostic value dysregulations of the Hippo genes in OC. Our data demonstrate the major role the conserved Hippo pathway presents in tumor control, underlying potential therapeutic strategies and controlling several steps modulated by miRNAs and their target genes that could limit ovarian cancer progression.
机译:河马信号通路,人类最保守的途径之一,控制器官和肿瘤生长的尺寸,经常在几种人类恶性肿瘤中造成危险,包括卵巢癌(OC)。据报道,河马信号传导的改变有助于卵巢癌发生和进展。然而,OC患者中单个河马基因的预后作用仍然难以捉摸。在此,我们研究了OC的关键河马基因的表达水平和预后价值使用在线数据库,其次是额外的患者队列中的QRT-PCR验证步骤。使用Gepia数据库,我们观察到TP53的增加水平,并降低了LAT1,LATS2,MST1,TAZ和肿瘤组织中的TAZ的表达水平与正常相邻组织。此外,Lats1,Lats2,TP53,TAZ和TEF表达水平具有预后意义与无进展的存活率相关。 QRT-PCR验证步骤在包含29个肿瘤组织和20个正常相邻组织的OC患者队列中进行,以支持LAT1,LATS2和TP53的表达水平,以及靶向TP53基因的两种miRNA,揭示MIR -25-3P上调和MIR-181C-5P下调。这些结果显示oc中存在河马基因的临界预后价值失效。我们的数据证明了保守的河马途径在肿瘤控制中提出的主要作用,潜在的治疗策略和控制MiRNA调节的几个步骤及其靶基因,可以限制卵巢癌进展。

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