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Size control in mammalian cells involves modulation of both growth rate and cell cycle duration

机译:哺乳动物细胞的大小控制涉及生长速率和细胞周期持续时间的调节

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摘要

Despite decades of research, how mammalian cell size is controlled remains unclear because of the difficulty of directly measuring growth at the single-cell level. Here we report direct measurements of single-cell volumes over entire cell cycles on various mammalian cell lines and primary human cells. We find that, in a majority of cell types, the volume added across the cell cycle shows little or no correlation to cell birth size, a homeostatic behavior called “adder”. This behavior involves modulation of G1 or S-G2 duration and modulation of growth rate. The precise combination of these mechanisms depends on the cell type and the growth condition. We have developed a mathematical framework to compare size homeostasis in datasets ranging from bacteria to mammalian cells. This reveals that a near-adder behavior is the most common type of size control and highlights the importance of growth rate modulation to size control in mammalian cells.
机译:尽管进行了数十年的研究,但由于难以直接测量单细胞水平的生长情况,如何控制哺乳动物细胞的大小仍不清楚。在这里,我们报告了在各种哺乳动物细胞系和原代人细胞上整个细胞周期中单细胞体积的直接测量。我们发现,在大多数细胞类型中,整个细胞周期增加的体积与细胞出生大小几乎没有或没有相关性,这种稳态行为称为“加法器”。此行为涉及对G1或S-G2持续时间的调节以及对增长率的调节。这些机制的精确组合取决于细胞类型和生长条件。我们开发了一个数学框架来比较从细菌到哺乳动物细胞的数据集中大小的稳态。这揭示了近加行为是尺寸控制的最常见类型,并突出了生长速率调节对哺乳动物细胞尺寸控制的重要性。

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