University of Navarra (UNAV). Center for Applied Medical Research (CIMA). Program of Gene Therapy and Hepatology. Pamplona, Spain.
UNAV/CIMA. Bioinformatics Platform. Pamplona, Spain.
Cancer Res. 2019 Oct 15;79(20):5167-5180. doi: 10.1158/0008-5472.CAN-19-0400. Epub 2019 Aug 6.
The Cancer Genome Atlas (TCGA) and Genotype-Tissue Expression (GTEx) datasets allow unprecedented gene expression analyses. Here, using these datasets, we performed pan-cancer and pan-tissue identification of coding and long noncoding RNA (lncRNA) transcripts differentially expressed in tumors and preferentially expressed in healthy tissues and/or tumors. Pan-cancer comparison of mRNAs and lncRNAs showed that lncRNAs were deregulated in a more tumor-specific manner. Given that lncRNAs are more tissue-specific than mRNAs, we identified healthy tissues that preferentially express lncRNAs upregulated in tumors and found that testis, brain, the digestive tract, and blood/spleen were the most prevalent. In addition, specific tumors also upregulate lncRNAs preferentially expressed in other tissues, generating a unique signature for each tumor type. Most tumors studied downregulated lncRNAs preferentially expressed in their tissue of origin, probably as a result of dedifferentiation. However, the same lncRNAs could be upregulated in other tumors, resulting in "bimorphic" transcripts. In hepatocellular carcinoma (HCC), the upregulated genes identified were expressed at higher levels in patients with worse prognosis. Some lncRNAs upregulated in HCC and preferentially expressed in healthy testis or brain were predicted to function as oncogenes and were significantly associated with higher tumor burden, and poor prognosis, suggesting their relevance in hepatocarcinogenesis and/or tumor evolution. Taken together, therapies targeting oncogenic lncRNAs should take into consideration the healthy tissue, where the lncRNAs are preferentially expressed, to predict and decrease unwanted secondary effects and increase potency. SIGNIFICANCE: Comprehensive analysis of coding and noncoding genes expressed in different tumors and normal tissues, which should be taken into account to predict side effects from potential coding and noncoding gene-targeting therapies. http://cancerres.aacrjournals.org/content/canres/79/20/5167/F1.large.jpg.
癌症基因组图谱(TCGA)和基因型组织表达(GTEx)数据集允许进行前所未有的基因表达分析。在这里,我们使用这些数据集,对肿瘤中差异表达且在健康组织和/或肿瘤中优先表达的编码和长非编码 RNA(lncRNA)转录本进行了泛癌和泛组织鉴定。mRNA 和 lncRNA 的泛癌比较表明,lncRNA 的失调更具有肿瘤特异性。鉴于 lncRNA 比 mRNA 更具组织特异性,我们鉴定了优先表达肿瘤上调 lncRNA 的健康组织,并发现睾丸、大脑、消化道和血液/脾脏最为常见。此外,特定的肿瘤也上调了优先在其他组织中表达的 lncRNA,为每种肿瘤类型生成了独特的特征。大多数研究的肿瘤下调了优先在其起源组织中表达的 lncRNA,可能是去分化的结果。然而,相同的 lncRNA 也可以在其他肿瘤中上调,导致“双态”转录本。在肝细胞癌(HCC)中,鉴定出的上调基因在预后较差的患者中表达水平更高。一些在 HCC 中上调且优先在健康睾丸或大脑中表达的 lncRNA 被预测为癌基因,与更高的肿瘤负担和不良预后显著相关,这表明它们在肝癌发生和/或肿瘤进化中的相关性。综上所述,针对致癌 lncRNA 的治疗方法应考虑到 lncRNA 优先表达的健康组织,以预测和减少不必要的副作用并提高效力。
对不同肿瘤和正常组织中表达的编码和非编码基因进行综合分析,这应该在考虑对潜在编码和非编码基因靶向治疗的副作用预测时予以考虑。
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