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人类转录因子在表达、调控、相互作用、表型和癌症生存方面的全面调查。

A comprehensive survey for human transcription factors on expression, regulation, interaction, phenotype and cancer survival.

机构信息

Center for Artificial Intelligence Biology, Hubei Bioinformatics and Molecular Imaging Key Laboratory, Key Laboratory of Molecular Biophysics of the Ministry of Education, College of Life Science and Technology, Huazhong University of Science and Technology, Wuhan 430074, China.

出版信息

Brief Bioinform. 2021 Sep 2;22(5). doi: 10.1093/bib/bbab002.

Abstract

Transcription factors (TFs) act as key regulators in biological processes through controlling gene expression. Here, we conducted a systematic study for all human TFs on the expression, regulation, interaction, mutation, phenotype and cancer survival. We revealed that the average expression levels of TFs in normal tissues were lower than 50% expression of non-TFs, whereas TF expression was increased in cancers. TFs that are specifically expressed in an individual tissue or cancer may be potential marker genes. For instance, TGIF2LX/Y were preferentially expressed in testis and NEUROG1, PRDM14, SRY, ZNF705A and ZNF716 were specifically highly expressed in germ cell tumors. We found different distributions of target genes and TF co-regulations in different TF families. Some small TF families have huge protein interaction pairs, suggesting their central roles in transcriptional regulation. The bZIP family is a small family involving many signaling pathways. Survival analysis indicated that most TFs significantly affect survival of one or more cancers. Some survival-related TFs were also specifically highly expressed in the corresponding cancer types, which may be potential targets for cancer therapy. Finally, we identified 43 TFs whose mutations were closely correlated to survival, suggesting their cancer-driven roles. The systematic analysis of TFs provides useful clues for further investigation of TF regulatory mechanisms and the role of TFs in diseases.

摘要

转录因子 (TFs) 通过控制基因表达在生物过程中充当关键调节剂。在这里,我们对所有人类 TFs 的表达、调控、相互作用、突变、表型和癌症生存进行了系统研究。我们揭示了 TFs 在正常组织中的平均表达水平低于非 TFs 的 50%,而在癌症中 TFs 的表达增加。在特定组织或癌症中特异性表达的 TFs 可能是潜在的标记基因。例如,TGIF2LX/Y 在睾丸中优先表达,而 NEUROG1、PRDM14、SRY、ZNF705A 和 ZNF716 在生殖细胞肿瘤中特异性高度表达。我们发现不同 TF 家族的靶基因和 TF 共同调控有不同的分布。一些小的 TF 家族具有巨大的蛋白质相互作用对,表明它们在转录调控中的核心作用。bZIP 家族是一个涉及许多信号通路的小家族。生存分析表明,大多数 TFs 显著影响一种或多种癌症的生存。一些与生存相关的 TFs 在相应的癌症类型中也特异性高度表达,这可能是癌症治疗的潜在靶点。最后,我们确定了 43 个 TFs,它们的突变与生存密切相关,表明它们在癌症中的驱动作用。对 TFs 的系统分析为进一步研究 TF 调节机制和 TFs 在疾病中的作用提供了有用的线索。

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