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基于肝内胆管癌的表达谱和miRNA-mRNA调控网络选择分子治疗药物靶点。

Selecting molecular therapeutic drug targets based on the expression profiles of intrahepatic cholangiocarcinomas and miRNA-mRNA regulatory networks.

作者信息

Sun Boshi, Xie Changming, Zheng Tongsen, Yin Dalong, Wang Jiabei, Liang Yingjian, Li Yuejin, Yang Guangchao, Shi Huawen, Pei Tiemin, Han Jihua, Liu Lianxin

机构信息

Key Laboratory of Hepatosplenic Surgery, Chinese Ministry of Education, Department of General Surgery, The First Affiliated Hospital of Harbin Medical University, Harbin, Heilongjiang 150001, P.R. China.

出版信息

Oncol Rep. 2016 Jan;35(1):382-90. doi: 10.3892/or.2015.4330. Epub 2015 Oct 15.

Abstract

The incidence of intrahepatic cholangiocarcinoma (ICC) is increasing yearly, making it the second most common carcinoma after hepatocellular carcinoma among primary malignant liver tumors. Integrated miRNA and mRNA analysis is becoming more frequently used in antitumor ICC treatment. However, this approach generates vast amounts of data, which leads to difficulties performing comprehensive analyses to identify specific therapeutic drug targets. In this study, we provide an in-depth analysis of ICC function, identifying potential highly potent antitumor drugs for antitumor therapy. Two sets of whole genome expression profiles were obtained from the Gene Expression Omnibus (GEO) database. Using modular bioinformatic analysis, six core functional modules were identified for ICC. Based on a Fisher's test of the Cmap small molecule drug database, 65 drug components were identified that regulated the genes of these six core modules. Literature mining was then used to identify 15 new potential antitumor drugs.

摘要

肝内胆管癌(ICC)的发病率逐年上升,使其成为原发性恶性肝肿瘤中仅次于肝细胞癌的第二常见癌症。整合的miRNA和mRNA分析在ICC抗肿瘤治疗中的应用越来越频繁。然而,这种方法会产生大量数据,导致难以进行全面分析以确定特定的治疗药物靶点。在本研究中,我们对ICC功能进行了深入分析,确定了潜在的高效抗肿瘤药物用于抗肿瘤治疗。从基因表达综合数据库(GEO)中获得了两组全基因组表达谱。使用模块化生物信息学分析,为ICC确定了六个核心功能模块。基于对Cmap小分子药物数据库的Fisher检验,确定了65种调节这六个核心模块基因的药物成分。然后通过文献挖掘确定了15种新的潜在抗肿瘤药物。

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