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泛癌症分析揭示了庇护体复合物在癌症中的调控和临床结局关联。

Pan-cancer analyses reveal regulation and clinical outcome association of the shelterin complex in cancer.

机构信息

Institute of Precision Medicine, The First Affiliated Hospital, Sun Yat-Sen University, Guangzhou, Guangdong 510080, China.

出版信息

Brief Bioinform. 2021 Sep 2;22(5). doi: 10.1093/bib/bbaa441.

Abstract

Shelterin, a protective complex at telomeres, plays essential roles in cancer. In addition to maintain telomere integrity, shelterin functions in various survival pathways. However, the detailed mechanisms of shelterin regulation in cancer remain elusive. Here, we perform a comprehensive analysis of shelterin in 9125 tumor samples across 33 cancer types using multi-omic data from The Cancer Genome Atlas, and validate some findings in Chinese Glioma Genome Atlas and cancer cell lines from Cancer Cell Line Encyclopedia. In the genomic landscape, we identify the amplification of TRF1 and POT1, co-amplification/deletion of TRF2-RAP1-TPP1 as the dominant alteration events. Clustering analysis based on shelterin expression reveals three cancer clusters with different degree of genome instability. To measure overall shelterin activity in cancer, we derive a shelterin score based on shelterin expression. Pathway analysis shows shelterin is positively correlated with E2F targets, while is negatively correlated with p53 pathway. Importantly, shelterin links to tumor immunity and predicts response to PD-1 blockade immune therapy. In-depth miRNA analysis reveals a miRNA-shelterin interaction network, with p53 regulated miRNAs targeting multiple shelterin components. We also identify a significant amount of lncRNAs regulating shelterin expression. In addition, we find shelterin expression could be used to predict patient survival in 24 cancer types. Finally, by mining the connective map database, we discover a number of potential drugs that might target shelterin. In summary, this study provides broad molecular signatures for further functional and therapeutic studies of shelterin, and also represents a systemic approach to characterize key protein complex in cancer.

摘要

端粒体保护复合物 Shelterin 在癌症中发挥着重要作用。除了维持端粒的完整性外,Shelterin 还在各种生存途径中发挥作用。然而,Shelterin 在癌症中的调节机制仍不清楚。在这里,我们使用来自癌症基因组图谱的多组学数据,对 33 种癌症类型的 9125 个肿瘤样本中的 Shelterin 进行了全面分析,并在中国脑胶质瘤基因组图谱和癌症细胞系百科全书的癌症细胞系中验证了一些发现。在基因组景观中,我们确定了 TRF1 和 POT1 的扩增,TRF2-RAP1-TPP1 的共扩增/缺失是主要的改变事件。基于 Shelterin 表达的聚类分析揭示了三种具有不同程度基因组不稳定性的癌症簇。为了衡量癌症中整体 Shelterin 活性,我们根据 Shelterin 表达推导了一个 Shelterin 评分。通路分析表明,Shelterin 与 E2F 靶标呈正相关,而与 p53 通路呈负相关。重要的是,Shelterin 与肿瘤免疫有关,并预测对 PD-1 阻断免疫治疗的反应。深入的 miRNA 分析揭示了一个 miRNA-Shelterin 相互作用网络,p53 调节的 miRNA 靶向多个 Shelterin 成分。我们还确定了大量调节 Shelterin 表达的 lncRNA。此外,我们发现 Shelterin 表达可用于预测 24 种癌症类型的患者生存。最后,通过挖掘连接图数据库,我们发现了一些可能靶向 Shelterin 的潜在药物。总之,这项研究为进一步研究 Shelterin 的功能和治疗提供了广泛的分子特征,也代表了一种系统的方法来描述癌症中的关键蛋白复合物。

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