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Application of intelligent algorithm in the optimization of novel protein regulatory pathway: Mechanism of action of gastric carcinoma protein p42.3

机译:智能算法在优化蛋白质新调控途径中的应用:胃癌蛋白p42.3的作用机理

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Aims: This purpose of the study was to optimize the regulatory mechanism of p42.3 novel protein molecule in gastric cancer and also verified it by the use of intelligent algorithms. Subjects and Methods: Threading method was employed to analyze structural domain characteristics of p42.3 protein. Referential proteins were gathered and formed by domain homology and function similarity. Afterwards, the possible regulatory network of p42.3 was established by analyzing the acting pathways of the referential proteins. Spherical polar coordinates stratification and stratified multi-parameter weight were used for calculation of the similarity between the referential proteins and p42.3 protein, the result of which was taken as the prior probability of the initial node in Bayes network, thus the probability of occurrence of each pathway was figured out by using conditional probability formula, and the one with the biggest probability was considered as the possible pathway of p42.3. At last, molecular biological experiments were conducted to verify it. Results: The acting pathway with the maximum probability predicted by Bayesian probability optimizing calculation was “S100A11” – RAGE – P38 – MAPK – Microtubule–associated protein – Spindle protein-Centromere protein – Cell proliferation” which was the most likely acting pathway participated by p42.3, and has been validated by biological experiments. Conclusions: By the theoretical analysis and experimental verification, this study confirmed that assumptions that p42.3 protein was related to the occurrence and development of gastric carcinoma, predicted and verified the acting pathways of p42.3, which will provide a new research direction of the relationship between p42.3 and gastric cancer, as well as the target therapy of gastric cancer. The algorithm in predicting the acting pathway of the protein also offers a new thought in studying new functional proteins.
机译:目的:本研究的目的是优化胃癌中p42.3新蛋白分子的调控机制,并通过智能算法对其进行验证。研究对象和方法:采用穿线法分析p42.3蛋白的结构域特征。通过域同源性和功能相似性收集并形成参照蛋白。之后,通过分析参考蛋白的作用途径,建立了可能的p42.3调控网络。球形极坐标分层和分层多参数权重用于计算参考蛋白质与p42.3蛋白质之间的相似性,其结果被认为是贝叶斯网络中初始节点的先验概率,因此是发生概率通过条件概率公式计算出每种途径的概率,将概率最大的途径视为p42.3的可能途径。最后,通过分子生物学实验对其进行了验证。结果:通过贝叶斯概率优化计算预测的最大可能性的作用途径是“ S100A11” – RAGE – P38 – MAPK –微管相关蛋白–主轴蛋白-着丝粒蛋白–细胞增殖,这是p42最有可能参与的作用途径.3,并已通过生物学实验验证。结论:通过理论分析和实验验证,本研究证实p42.3蛋白与胃癌的发生,发展有关的假设,预测并验证了p42.3的作用途径,将为p42.3的研究提供新的方向。 p42.3与胃癌的关系以及胃癌的靶向治疗。预测蛋白质作用途径的算法也为研究新功能蛋白质提供了新思路。

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