ZC3H12A在结直肠癌不同分期中的表达

Oncoscience Pub Date : 2019-04-02 eCollection Date: 2019-03-01 DOI:10.18632/oncoscience.480
Tao Chen, Di Du, Jian Chen, Pinghong Zhou, John N Weinstein, Liqing Yao, Yuexin Liu
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引用次数: 9

摘要

早期结直肠癌患者的识别为治疗性局部切除提供了机会。然而,用于I期肿瘤预测的可靠标志物尚未开发。我们使用TCGA数据集分析了221例CRC样本的rna测序数据,以确定I期CRC的新生物标志物。接下来,我们在290例CRC患者的独立GEO队列和110例CRC肿瘤和匹配正常样本的第三个队列中验证了TCGA的发现。进一步分析ZC3H12A基因表达与临床病理特征及无病生存的相关性。ZC3H12A与趋化因子配体的表达相关性通过Student’st检验。在TCGA队列中,I期CRC患者的ZC3H12A mRNA表达明显高于其他三个阶段的合并,并与其他单个阶段呈两两关系(P
本文章由计算机程序翻译,如有差异,请以英文原文为准。

ZC3H12A Expression in Different Stages of Colorectal Cancer.

ZC3H12A Expression in Different Stages of Colorectal Cancer.

ZC3H12A Expression in Different Stages of Colorectal Cancer.

ZC3H12A Expression in Different Stages of Colorectal Cancer.

Identification of CRC patients with early-stage disease provides the opportunity for curative local resection. However, robust markers for stage I tumor prediction are yet to be developed. We analyzed RNA-sequencing data of 221 CRC samples using the TCGA dataset to identify novel biomarkers for stage I CRC. We next validated the TCGA finding in an independent GEO cohort of 290 CRC patients and in a third cohort of 110 CRC tumors and matched normal samples. We further performed correlative analysis of ZC3H12A gene expression with clinicopathologic features and disease-free survival. Expression correlation of ZC3H12A with the chemokine ligands was evaluated via Student's t-test. In the TCGA cohort, stage I CRC patients had significantly higher ZC3H12A mRNA expression as compared with the other three stages combined and with the other individual stages in a pairwise manner (P<0.001 for all comparisons). The significant association of ZC3H12A gene expression with stages was further validated in the GEO cohort and in the additional third cohort. In support of these findings, we further found that patients with lower ZC3H12A expression had more aggressive tumor features and shorter disease-free survival. Biologically, ZC3H12A expression was significantly correlated with expression of three chemokine ligands (CXCL1, CXCL2 and CXCL3), suggesting that immune response dysregulation likely contributes to CRC development. Our results demonstrate ZC3H12A's potential role in identification of CRC patients with early-stage disease.

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