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Analyzing the dynamics of cell cycle processes from fixed samples through ergodic principles

机译:通过遍历原理分析固定样本中细胞周期过程的动力学

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摘要

Tools to analyze cyclical cellular processes, particularly the cell cycle, are of broad value for cell biology. Cell cycle synchronization and live-cell time-lapse observation are widely used to analyze these processes but are not available for many systems. Simple mathematical methods built on the ergodic principle are a well-established, widely applicable, and powerful alternative analysis approach, although they are less widely used. These methods extract data about the dynamics of a cyclical process from a single time-point "snapshot" of a population of cells progressing through the cycle asynchronously. Here, I demonstrate application of these simple mathematical methods to analysis of basic cyclical processes-cycles including a division event, cell populations undergoing unicellular aging, and cell cycles with multiple fission (schizogony)-as well as recent advances that allow detailed mapping of the cell cycle from continuously changing properties of the cell such as size and DNA content. This includes examples using existing data from mammalian, yeast, and unicellular eukaryotic parasite cell biology. Through the ongoing advances in high-throughput cell analysis by light microscopy, electron microscopy, and flow cytometry, these mathematical methods are becoming ever more important and are a powerful complementary method to traditional synchronization and time-lapse cell cycle analysis methods.
机译:分析周期性细胞过程特别是细胞周期的工具对于细胞生物学具有广泛的价值。细胞周期同步和活细胞延时观察已广泛用于分析这些过程,但不适用于许多系统。尽管遍历原理不那么广泛,但基于遍历原理的简单数学方法是一种行之有效,广泛应用且功能强大的替代分析方法。这些方法从异步进行循环的一组细胞的单个时间点“快照”中提取有关循环过程动力学的数据。在这里,我演示了这些简单的数学方法在分析基本循环过程中的应用,这些循环包括分裂事件,经历单细胞衰老的细胞群体以及具有多重裂变(分裂)的细胞周期,以及最近的进展(允许对这些过程进行详细的定位)不断变化的细胞特性(例如大小和DNA含量)引起的细胞周期。这包括使用来自哺乳动物,酵母和单细胞真核寄生虫细胞生物学的现有数据的示例。通过光学显微镜,电子显微镜和流式细胞术在高通量细胞分析方面的不断发展,这些数学方法变得越来越重要,并且是传统同步和延时细胞周期分析方法的有力补充。

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