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A genomic multiprocess survey of machineries that control and link cell shape, microtubule organization, and cell-cycle progression

机译:控制和链接细胞形状,微管组织和细胞周期进程的机器的基因组多过程调查

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摘要

Understanding cells as integrated systems requiresthat we systematically decipher how single genesaffect multiple biological processes and how processes are functionally linked. Here, we used multiprocess phenotypic profiling, combining high-resolution 3D confocal microscopy and multiparametric image analysis, to simultaneously survey the fission yeast genome with respect to three key cellular processes: cell shape, microtubule organization, and cell-cycle progression. We identify, validate, and functionally annotate 262 genes controlling specific aspects of those processes. Of these, 62% had not been linked to these processes before and 35% are implicated in multiple processes. Importantly, we identify a conserved role for DNA-damage responses in controlling microtubule stability. In addition, we investigate how the processes are functionally linked. We show unexpectedly that disruption of cell-cycle progression does not necessarily affect cell size control and that distinct aspects of cell shape regulate microtubules and vice versa, identifying important systems-level links across these processes.
机译:将细胞理解为集成系统要求我们系统地解读单个基因如何影响多个生物学过程以及过程之间的功能联系。在这里,我们使用了多过程表型分析,结合了高分辨率3D共聚焦显微镜和多参数图像分析,就三个关键细胞过程同时观察了裂变酵母基因组:细胞形状,微管组织和细胞周期进程。我们确定,验证和功能注释262个基因,这些基因控制着这些过程的特定方面。其中,有62%的人以前未与这些过程相关联,而35%的人涉及多个过程。重要的是,我们确定了DNA损伤反应在控制微管稳定性中的保守作用。此外,我们研究了流程之间的功能联系。我们出乎意料地表明,细胞周期进程的破坏并不一定会影响细胞大小的控制,并且细胞形状的不同方面会调节微管,反之亦然,从而确定了这些过程中重要的系统级联系。

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