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首页> 外文期刊>Computational and mathematical methods in medicine >Optimization and Corroboration of the Regulatory Pathway of p42.3 Protein in the Pathogenesis of Gastric Carcinoma
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Optimization and Corroboration of the Regulatory Pathway of p42.3 Protein in the Pathogenesis of Gastric Carcinoma

机译:P42.3蛋白调节途径在胃癌发病机制中的优化与腐蚀

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摘要

Aims. To optimize and verify the regulatory pathway of p42.3 in the pathogenesis of gastric carcinoma (GC) by intelligent algorithm.Methods. Bioinformatics methods were used to analyze the features of structural domain in p42.3 protein. Proteins with the same domains and similar functions to p42.3 were screened out for reference. The possible regulatory pathway of p42.3 was established by integrating the acting pathways of these proteins. Then, the similarity between the reference proteins and p42.3 protein was figured out by multiparameter weighted summation method. The calculation result was taken as the prior probability of the initial node in Bayesian network. Besides, the probability of occurrence in different pathways was calculated by conditional probability formula, and the one with the maximum probability was regarded as the most possible pathway of p42.3. Finally, molecular biological experiments were conducted to prove it.Results. In Bayesian network of p42.3, probability of the acting pathway “S100A11→RAGE→P38→MAPK→Microtubule-associated protein→Spindle protein→Centromere protein→Cell proliferation” was the biggest, and it was also validated by biological experiments.Conclusions. The possibly important role of p42.3 in the occurrence of gastric carcinoma was verified by theoretical analysis and preliminary test, helping in studying the relationship between p42.3 and gastric carcinoma.
机译:目标。通过智能算法优化和验证P42.3的调节途径。方法。生物信息学方法用于分析P42.3蛋白中结构结构域的特征。筛选出具有相同结构域的蛋白质和与P42.3类似的功能以供参考。通过整合这些蛋白质的作用途径来建立P42.3可能的调节途径。然后,通过多游ameter加权求和方法对参考蛋白和P42.3蛋白质之间的相似性。计算结果作为贝叶斯网络中初始节点的现有概率。此外,通过条件概率公式计算不同途径的发生概率,并且具有最大概率的概率被认为是最可能的P42.3途径。最后,进行了分子生物实验以证明它。结果。在P42.3的贝叶斯网络中,作用途径的概率“S100A11→RAGE→P38→MAPK→MICROUBULE相关蛋白→主轴蛋白→CENTROMERE蛋白→细胞增殖”是最大的,它也是通过生物实验验证的.CONCLUSIONS 。 P42.3在理论分析和初步试验中验证了P42.3在发生胃癌的发生中可能重要的作用,有助于研究P42.3与胃癌的关系。

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