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肿瘤发生中遗传和通路改变的时间顺序。

The temporal order of genetic and pathway alterations in tumorigenesis.

机构信息

Department of Biosystems Science and Engineering, ETH Zurich, Basel, Switzerland.

出版信息

PLoS One. 2011;6(11):e27136. doi: 10.1371/journal.pone.0027136. Epub 2011 Nov 1.

Abstract

Cancer evolves through the accumulation of mutations, but the order in which mutations occur is poorly understood. Inference of a temporal ordering on the level of genes is challenging because clinically and histologically identical tumors often have few mutated genes in common. This heterogeneity may at least in part be due to mutations in different genes having similar phenotypic effects by acting in the same functional pathway. We estimate the constraints on the order in which alterations accumulate during cancer progression from cross-sectional mutation data using a probabilistic graphical model termed Hidden Conjunctive Bayesian Network (H-CBN). The possible orders are analyzed on the level of genes and, after mapping genes to functional pathways, also on the pathway level. We find stronger evidence for pathway order constraints than for gene order constraints, indicating that temporal ordering results from selective pressure acting at the pathway level. The accumulation of changes in core pathways differs among cancer types, yet a common feature is that progression appears to begin with mutations in genes that regulate apoptosis pathways and to conclude with mutations in genes involved in invasion pathways. H-CBN models provide a quantitative and intuitive model of tumorigenesis showing that the genetic events can be linked to the phenotypic progression on the level of pathways.

摘要

癌症是通过突变的积累而演变的,但突变发生的顺序还不太清楚。在基因水平上推断时间顺序是具有挑战性的,因为临床上和组织学上相同的肿瘤通常很少有共同的突变基因。这种异质性至少部分是由于不同基因中的突变通过在相同的功能途径中起作用而具有相似的表型效应。我们使用一种称为隐藏联合贝叶斯网络(H-CBN)的概率图形模型,从横截面突变数据中估计癌症进展过程中突变积累的顺序约束。对基因水平和将基因映射到功能途径后的途径水平进行可能的顺序分析。我们发现,与基因顺序约束相比,途径顺序约束具有更强的证据,这表明时间顺序是由作用于途径水平的选择性压力引起的。核心途径中变化的积累在不同的癌症类型之间存在差异,但一个共同的特征是,进展似乎始于调节细胞凋亡途径的基因中的突变,并以涉及侵袭途径的基因中的突变结束。H-CBN 模型提供了一种肿瘤发生的定量和直观模型,表明遗传事件可以与途径水平的表型进展相关联。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/dc86/3206070/3ada6507e61c/pone.0027136.g001.jpg

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