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计算机模拟通路重建:酿酒酵母中的铁硫簇生物合成

In silico pathway reconstruction: Iron-sulfur cluster biogenesis in Saccharomyces cerevisiae.

作者信息

Alves Rui, Sorribas Albert

机构信息

Departament de Ciencies Mediques Basiques, Universidad de Lleida, Montserrat Roig 2, 25008 Lleida, Spain.

出版信息

BMC Syst Biol. 2007 Jan 31;1:10. doi: 10.1186/1752-0509-1-10.

Abstract

BACKGROUND

Current advances in genomics, proteomics and other areas of molecular biology make the identification and reconstruction of novel pathways an emerging area of great interest. One such class of pathways is involved in the biogenesis of Iron-Sulfur Clusters (ISC).

RESULTS

Our goal is the development of a new approach based on the use and combination of mathematical, theoretical and computational methods to identify the topology of a target network. In this approach, mathematical models play a central role for the evaluation of the alternative network structures that arise from literature data-mining, phylogenetic profiling, structural methods, and human curation. As a test case, we reconstruct the topology of the reaction and regulatory network for the mitochondrial ISC biogenesis pathway in S. cerevisiae. Predictions regarding how proteins act in ISC biogenesis are validated by comparison with published experimental results. For example, the predicted role of Arh1 and Yah1 and some of the interactions we predict for Grx5 both matches experimental evidence. A putative role for frataxin in directly regulating mitochondrial iron import is discarded from our analysis, which agrees with also published experimental results. Additionally, we propose a number of experiments for testing other predictions and further improve the identification of the network structure.

CONCLUSION

We propose and apply an iterative in silico procedure for predictive reconstruction of the network topology of metabolic pathways. The procedure combines structural bioinformatics tools and mathematical modeling techniques that allow the reconstruction of biochemical networks. Using the Iron Sulfur cluster biogenesis in S. cerevisiae as a test case we indicate how this procedure can be used to analyze and validate the network model against experimental results. Critical evaluation of the obtained results through this procedure allows devising new wet lab experiments to confirm its predictions or provide alternative explanations for further improving the models.

摘要

背景

基因组学、蛋白质组学和分子生物学其他领域的当前进展使得新型途径的识别和重建成为一个备受关注的新兴领域。铁硫簇(ISC)生物合成所涉及的途径就是其中一类。

结果

我们的目标是开发一种基于数学、理论和计算方法的使用与结合的新方法,以识别目标网络的拓扑结构。在这种方法中,数学模型在评估从文献数据挖掘、系统发育谱分析、结构方法和人工编目中产生的替代网络结构方面发挥着核心作用。作为一个测试案例,我们重建了酿酒酵母中线粒体ISC生物合成途径的反应和调控网络的拓扑结构。通过与已发表的实验结果进行比较,验证了关于蛋白质在ISC生物合成中作用的预测。例如,Arh1和Yah1的预测作用以及我们对Grx5预测的一些相互作用都与实验证据相符。我们的分析摒弃了frataxin在直接调节线粒体铁导入方面的假定作用,这也与已发表的实验结果一致。此外,我们提出了一些实验来测试其他预测,并进一步改进网络结构的识别。

结论

我们提出并应用了一种迭代的计算机模拟程序,用于代谢途径网络拓扑结构的预测重建。该程序结合了结构生物信息学工具和数学建模技术,能够重建生化网络。以酿酒酵母中的铁硫簇生物合成作为测试案例,我们展示了该程序如何用于根据实验结果分析和验证网络模型。通过该程序对所得结果进行批判性评估,有助于设计新的湿实验室实验,以确认其预测结果或为进一步改进模型提供替代解释。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/4f1e/1839888/35508da8a59d/1752-0509-1-10-1.jpg

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