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Characteristics and prognostic value of potential dependency genes in clear cell renal cell carcinoma based on a large-scale CRISPR-Cas9 and RNAi screening database DepMap

机译:基于大规模CRAP-CAS9和RNAI筛选数据库DEPAP的透明细胞肾细胞癌潜在依赖基因的特征及预测值

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Background: Large-scale loss-of-function screening database such as Cancer Dependency Map (Depmap) provide abundant resources. Investigation of these potential dependency genes from human cancer cell lines in the real-world patients cohort would evaluate their prognostic value thus facilitate their clinical application and guide drug development. Methods: A few genes were selected from top clear cell renal cell carcinoma (ccRCC) lineage preferential dependency candidates from Depmap. Their characteristic including expression levels both in normal and tumor tissues and correlations with methylation or copy number, genetic alterations, functional enrichment, immune-associated interactions, prognostic value were evaluated in KIRC cohort from TCGA, GTEx, and multiple other open databases and platforms. Results: 16 genes were collected from 106 ccRCC preferential candidates and further analyzed including B4GALT4, BCL2L1, CDH2, COPG1, CRB3, FERMT2, GET4, GPX4, HNF1B, ITGAV, MDM2, NFE2L2, PAX8, RUVBL1, TFRC, and TNFSF10. The normalized gene effect scores of these genes varied from different ccRCC cell lines and principal component analysis (PCA) showed their tissue specificity expression profiles. Genetic alteration rates of them were low to moderate (0.7%-13%) in KIRC cohort. CDH2, MDM2, TNFSF10 showed a statistically significant higher level in tumors than normal tissues while PAX8 and FERMT2 were significantly downregulated. Moderate positive or negative correlations were observed in several genes between their expression and relative gene copy number or methylation levels, respectively. Based on the multivariable COX regression model adjusted by critical clinical variables revealed the expression of GET4 (p=0.002, HR=1.023 95%CI 1.009-1.038) and CRB3 (p0.001, HR=0.969 95%CI 0.960-0.980) were independent predictive factors for overall survival in KIRC cohort. Conclusions: A dependency gene validated in cell lines didn't directly represent its role in corresponding patients with same histological type and their prognostic value might be determined by multiple factors including dependency driven types, genetic alteration rates and expression levels. GET4 and CRB3 were the independent prognostic factors for ccRCC patients. CRB3 seemed like a potential broad tumor suppressor gene while GET4 might be a ccRCC preferential dependency gene with a ligandable structure.
机译:背景:诸如癌症依赖图(DEPMAP)的大规模丢失筛选数据库提供丰富的资源。从现实世界患者队列中的人癌细胞系中这些潜在依赖基因的调查将评估其预后价值,从而促进其临床应用和指导药物发育。方法:从Depmap的顶部透明细胞肾细胞癌(CCRCC)谱系中选择少数基因。它们的特征包括正常和肿瘤组织中的表达水平和与甲基化或拷贝数,遗传改变,功能性富集,免疫相关的相互作用,在来自TCGA,GTEX和多个其他开放数据库和平台的kirc队列中评估了预后值。结果:从106个CCRCC优先考生收集16个基因,进一步分析,包括B4GALT4,BCL2L1,CDH2,COPG1,CRB3,FERMT2,GET4,GPX4,HNF1B,ITGAV,MDM2,NFE2L2,PAX8,RUVBL1,TFRC和TNFSF10。这些基因的标准化基因效应评分因不同CCRCC细胞系和主成分分析(PCA)而变化,显示了它们的组织特异性表达谱。它们的遗传改变率低于kirc队列中的中等(0.7%-13%)。 CDH2,MDM2,TNFSF10在肿瘤中显示出比正常组织在肿瘤上的统计学上显着的更高水平,而PAX8和FERMT2显着下调。在其表达和相对基因拷贝数或甲基化水平之间的几个基因中观察到中度正或负相关。基于通过关键临床变量调整的多变量Cox回归模型显示Get4的表达(P = 0.002,HR = 1.023 95%CI 1.009-1.038)和CRB3(P <0.001,HR = 0.969 95%CI 0.960-0.980) KIRC队列全面存活的独立预测因素。结论:在细胞系中验证的依赖性基因没有直接代表其在相同组织学类型的相应患者中的作用,并且它们的预后值可能由包括依赖性驱动类型,遗传改变率和表达水平的多种因素来确定。 GET4和CRB3是CCRCC患者的独立预后因素。 CRB3似乎是潜在的宽肿瘤抑制基因,而GET4可能是具有韧带结构的CCRCC优先依赖基因。

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