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Phenotypic clustering of yeast mutants based on kinetochore microtubule dynamics

机译:基于动粒微管动力学的酵母突变体表型聚类

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Motivation: Kinetochores are multiprotein complexes which mediate chromosome attachment to microtubules (MTs) of the mitotic spindle. They regulate MT dynamics during chromosome segregation. Our goal is to identify groups of kinetochore proteins with similar effects on MT dynamics, revealing pathways through which kinetochore proteins transform chemical and mechanical input signals into cues of MT regulation.Results: We have developed a hierarchical, agglomerative clustering algorithm that groups Saccharomyces cerevisiae strains based on MT-mediated chromosome dynamics measured by high-resolution live cell microscopy. Clustering is based on parameters of autoregressive moving average (ARMA) models of the probed dynamics. We have found that the regulation of wildtype MT dynamics varies with cell cycle and temperature, but not with the chromosome an MT is attached to. By clustering the dynamics of mutants, we discovered that the three genes IPL1, DAM1 and KIP3 co-regulate MT dynamics. Our study establishes the clustering of chromosome and MT dynamics by ARMA descriptors as a sensitive framework for the systematic identification of kinetochore protein subcomplexes and pathways for the regulation of MT dynamics.
机译:动机:动植物是多蛋白复合物,介导染色体附着在有丝分裂纺锤体的微管(MT)上。它们在染色体分离过程中调节MT动力学。我们的目标是鉴定对MT动力学具有相似影响的线粒体蛋白组,揭示线粒体蛋白将化学和机械输入信号转化为MT调控线索的途径。结果:我们开发了一种层次化的聚类聚类算法,对酿酒酵母菌株进行分组基于高分辨率活细胞显微镜测量的MT介导的染色体动力学。聚类基于所探测动态的自回归移动平均(ARMA)模型的参数。我们发现野生型MT动力学的调控随细胞周期和温度而变化,但与MT所附着的染色体无关。通过聚类突变体的动力学,我们发现三个基因IPL1,DAM1和KIP3共同调节MT动力学。我们的研究通过ARMA描述子建立了染色体和MT动态的聚类,将其作为系统识别动线粒体蛋白亚复合物和调节MT动态的途径的敏感框架。

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