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基于多数据库挖掘的 ABL1 基因与肝癌分子靶向药物的综合转录组学和共表达分析。

Comprehensive transcriptomic and co-expression analysis of ABL1 gene and molecularly targeted drugs in hepatocellular carcinoma based on multi-database mining.

机构信息

Medical Genetics Center, Guangdong Women and Children Hospital, Guangzhou, China.

Zhu's Team, Guangdong Medical University, Zhanjiang, China.

出版信息

Med Oncol. 2022 Jul 14;39(10):146. doi: 10.1007/s12032-022-01730-y.

Abstract

Hepatocellular carcinoma (HCC) is one of the leading causes of cancer death worldwide. Consequently, it is essential to identify biomarkers for treatment response and the prognosis prediction. We investigated whether ABL1 can function as a biomarker or a drug target for HCC. We assessed the ABL1 expression, genetic alterations and patients' survival from LinkedOmics, GEO, TCGA and Human Protein Atlas. We analyzed PPI, GO and KEGG pathways. GSEA was analyzed for functional comparison. The current drugs targeting ABL1 were statistically analyzed using DRUGSURV and DGIdb database. We found ABL1 is overexpressed in HCC and its higher expression reduces survival probability. Genetic changes of ABL1 are not frequent. We screened out 25 differentially expressed genes correlated with ABL1. The top functions of ABL1 are biological regulation, metabolic process, protein-containing, and protein binding. KEGG pathways showed that ABL1 and correlated with ABL1 significantly genes markedly enriched in the ErbB signaling pathway, and pathways in cancer. We counted the existing drugs targeting ABL1, which indicates that inhibiting ABL1 expression may improve the survival probability of HCC. In conclusion, ABL1 plays a crucial role in the development and progression of this cancerization and is a potential drug target.

摘要

肝细胞癌 (HCC) 是全球癌症死亡的主要原因之一。因此,识别治疗反应和预后预测的生物标志物至关重要。我们研究了 ABL1 是否可以作为 HCC 的生物标志物或药物靶点。我们从 LinkedOmics、GEO、TCGA 和 Human Protein Atlas 评估了 ABL1 的表达、遗传改变和患者的生存情况。我们分析了 PPI、GO 和 KEGG 途径。使用 DRUGSURV 和 DGIdb 数据库对 GSEA 进行了功能比较分析。我们发现 ABL1 在 HCC 中过表达,其高表达降低了生存概率。ABL1 的遗传变化并不频繁。我们筛选出与 ABL1 相关的 25 个差异表达基因。ABL1 的主要功能是生物调节、代谢过程、蛋白质包含和蛋白质结合。KEGG 途径显示,ABL1 与 ErbB 信号通路和癌症途径显著相关。我们计算了现有的针对 ABL1 的药物,这表明抑制 ABL1 的表达可能会提高 HCC 的生存概率。总之,ABL1 在这种癌变的发生和发展中起着关键作用,是一个潜在的药物靶点。

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