Cell growth dilutes the cell cycle inhibitor Rb to trigger cell division

细胞周期 细胞分裂 细胞生物学 细胞生长 细胞 细胞器 有丝分裂 限制点 师(数学) 细胞周期检查点 生物 细胞周期进展 化学 细胞培养 生物化学 遗传学 细胞周期蛋白依赖激酶
作者
Evgeny Zatulovskiy,Daniel F. Berenson,Benjamin R. Topacio,Jan M. Skotheim
标识
DOI:10.1101/470013
摘要

Cell size is fundamental to function in different cell types across the human body because it sets the scale of organelle structures, biosynthesis, and surface transport 1,2 . Tiny erythrocytes squeeze through capillaries to transport oxygen, while the million-fold larger oocyte divides without growth to form the ~100 cell pre-implantation embryo. Despite the vast size range across cell types, cells of a given type are typically uniform in size likely because cells are able to accurately couple cell growth to division 3–6 . While some genes whose disruption in mammalian cells affects cell size have been identified, the molecular mechanisms through which cell growth drives cell division have remained elusive 7–12 . Here, we show that cell growth acts to dilute the cell cycle inhibitor Rb to drive cell cycle progression from G1 to S phase in human cells. In contrast, other G1/S regulators remained at nearly constant concentration. Rb is a stable protein that is synthesized during S and G2 phases in an amount that is independent of cell size. Equal partitioning to daughter cells of chromatin bound Rb then ensures that all cells at birth inherit a similar amount of Rb protein. RB overexpression increased cell size in tissue culture and a mouse cancer model, while RB deletion decreased cell size and removed the inverse correlation between cell size at birth and the duration of G1 phase. Thus, Rb-dilution by cell growth in G1 provides a long-sought cell autonomous molecular mechanism for cell size homeostasis.

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