Exact and Approximate Stochastic Simulations of the MAPK Pathway and Comparisons of Simulations Results

J. Integr. Bioinform. Pub Date : 1900-01-01 DOI:10.2390/biecoll-jib-2006-38

Vilda Purutçuoglu Gazi, E. Wit

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引用次数: 3

Abstract

The MAPK (mitogen-activated protein kinase) or its synonymous ERK (extracellular signal regulated kinase) pathway whose components are Ras, Raf, and MEK proteins with many biochemical links, is one of the major signalling systems involved in cellular growth control of eukaryotes including cell proliferation, transformation, differentiation, and apoptosis. In this study we describe the MAPK/ERK pathway via (quasi) biochemical reactions and then implement the pathway by a stochastic Markov process. A novelty of our approach is to use multiple parametrizations in order to deal with molecules for which localization in the cell is an intricate part of the dynamic process and to describe the protein using different binding sites and various phosphorylations. We simulate the system by exact and different approximate simulations, e.g. via the Poisson τ -leap, the Binomial τ leap and the diffusion methods, in which we introduce a new updating plan for dependent columns of the diffusion matrix. Finally we compare the results of different algorithms by the current biological knowledge and find out new relations about this complex system.

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MAPK路径的精确和近似随机模拟及模拟结果比较

MAPK(丝裂原活化蛋白激酶)或其同义的ERK(细胞外信号调节激酶)通路由Ras、Raf和MEK蛋白组成，具有许多生化联系，是真核生物细胞生长控制的主要信号系统之一，包括细胞增殖、转化、分化和凋亡。在本研究中，我们通过(准)生化反应描述MAPK/ERK途径，然后通过随机马尔可夫过程实现该途径。我们的方法的一个新颖之处在于使用多个参数化来处理分子，这些分子在细胞中的定位是动态过程的一个复杂部分，并使用不同的结合位点和各种磷酸化来描述蛋白质。通过泊松τ -跃、二项式τ -跃和扩散方法对系统进行了精确和不同的近似模拟，并引入了扩散矩阵相关列的更新方案。最后利用现有的生物学知识对不同算法的结果进行了比较，发现了这个复杂系统的新关系。

本文章由计算机程序翻译，如有差异，请以英文原文为准。

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J. Integr. Bioinform.

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