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癌症中融合蛋白的分子特征

Molecular Signatures of Fusion Proteins in Cancer.

作者信息

Latysheva Natasha S, Babu M Madan

机构信息

MRC Laboratory of Molecular Biology, Francis Crick Avenue, Cambridge CB2 0QH, United Kingdom.

出版信息

ACS Pharmacol Transl Sci. 2019 Mar 20;2(2):122-133. doi: 10.1021/acsptsci.9b00019. eCollection 2019 Apr 12.

Abstract

Although gene fusions are recognized as driver mutations in a wide variety of cancers, the general molecular mechanisms underlying oncogenic fusion proteins are insufficiently understood. Here, we employ large-scale data integration and machine learning and (1) identify three functionally distinct subgroups of gene fusions and their molecular signatures; (2) characterize the cellular pathways rewired by fusion events across different cancers; and (3) analyze the relative importance of over 100 structural, functional, and regulatory features of ∼2200 gene fusions. We report subgroups of fusions that likely act as driver mutations and find that gene fusions disproportionately affect pathways regulating cellular shape and movement. Although fusion proteins are similar across different cancer types, they affect cancer type-specific pathways. Key indicators of fusion-forming proteins include high and nontissue specific expression, numerous splice sites, and higher centrality in protein-interaction networks. Together, these findings provide unifying and cancer type-specific trends across diverse oncogenic fusion proteins.

摘要

尽管基因融合被认为是多种癌症中的驱动突变,但致癌融合蛋白背后的一般分子机制仍未得到充分理解。在这里,我们采用大规模数据整合和机器学习,(1) 识别基因融合的三个功能不同的亚组及其分子特征;(2) 描述不同癌症中融合事件重新连接的细胞途径;(3) 分析约2200个基因融合的100多个结构、功能和调控特征的相对重要性。我们报告了可能作为驱动突变的融合亚组,并发现基因融合对调节细胞形状和运动的途径影响尤为显著。尽管融合蛋白在不同癌症类型中相似,但它们会影响特定癌症类型的途径。融合形成蛋白的关键指标包括高表达且非组织特异性表达、众多剪接位点以及在蛋白质相互作用网络中更高的中心性。这些发现共同揭示了不同致癌融合蛋白的统一趋势以及特定癌症类型的趋势。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/5a01/7088938/9db69dfdc5ca/pt-2019-000196_0001.jpg

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