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A Developmental Systems Perspective on Epistasis: Computational Exploration of Mutational Interactions in Model Developmental Regulatory Networks

机译:上位性的发展系统视角:模型发展监管网络中的相互作用的计算探索。

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摘要

The way in which the information contained in genotypes is translated into complex phenotypic traits (i.e. embryonic expression patterns) depends on its decoding by a multilayered hierarchy of biomolecular systems (regulatory networks). Each layer of this hierarchy displays its own regulatory schemes (i.e. operational rules such as +/− feedback) and associated control parameters, resulting in characteristic variational constraints. This process can be conceptualized as a mapping issue, and in the context of highly-dimensional genotype-phenotype mappings (GPMs) epistatic events have been shown to be ubiquitous, manifested in non-linear correspondences between changes in the genotype and their phenotypic effects. In this study I concentrate on epistatic phenomena pervading levels of biological organization above the genetic material, more specifically the realm of molecular networks. At this level, systems approaches to studying GPMs are specially suitable to shed light on the mechanistic basis of epistatic phenomena. To this aim, I constructed and analyzed ensembles of highly-modular (fully interconnected) networks with distinctive topologies, each displaying dynamic behaviors that were categorized as either arbitrary or functional according to early patterning processes in the Drosophila embryo. Spatio-temporal expression trajectories in virtual syncytial embryos were simulated via reaction-diffusion models. My in silico mutational experiments show that: 1) the average fitness decay tendency to successively accumulated mutations in ensembles of functional networks indicates the prevalence of positive epistasis, whereas in ensembles of arbitrary networks negative epistasis is the dominant tendency; and 2) the evaluation of epistatic coefficients of diverse interaction orders indicates that, both positive and negative epistasis are more prevalent in functional networks than in arbitrary ones. Overall, I conclude that the phenotypic and fitness effects of multiple perturbations are strongly conditioned by both the regulatory architecture (i.e. pattern of coupled feedback structures) and the dynamic nature of the spatio-temporal expression trajectories displayed by the simulated networks.
机译:基因型中包含的信息被转换为复杂的表型特征(即胚胎表达模式)的方式取决于其对生物分子系统(调控网络)的多层层次结构的解码。该层次结构的每一层都显示其自己的调节方案(即诸如+/-反馈之类的操作规则)和相关的控制参数,从而导致特征变化约束。可以将这一过程概念化为一个映射问题,并且在高维基因型-表型映射(GPM)的背景下,上位事件已被证明是普遍存在的,表现为基因型变化及其表型效应之间的非线性对应关系。在这项研究中,我集中研究遍及遗传物质之上的生物组织水平的上位现象,更具体地说是分子网络领域。在这个级别上,研究GPM的系统方法特别适合于根据上位现象的机理来阐明。为此,我构建并分析了具有独特拓扑结构的高度模块化(完全互连)网络的集合,每个网络都显示了根据果蝇胚胎早期构图过程分类为任意行为或功能行为的动态行为。通过反应扩散模型模拟了虚拟合胞体胚胎中的时空表达轨迹。我在计算机上进行的突变实验表明:1)功能网络集合中连续积累的突变的平均适应度衰减趋势表明阳性上位性流行,而任意网络集合中阴性上位性是主要趋势; 2)对各种相互作用顺序的上位系数的评估表明,在功能网络中,正向和负向上位性都比任意网络更普遍。总的来说,我得出结论,多重扰动的表型和适应性效应都受到监管体系结构(即耦合反馈结构的模式)和由模拟网络显示的时空表达轨迹的动态特性的强烈制约。

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    Gutiérrez, Jayson;

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  • 年度 2009
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  • 原文格式 PDF
  • 正文语种 {"code":"en","name":"English","id":9}
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