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Merck

Molecular control of cell density-mediated exit to quiescence.

Cell reports (2021-07-29)
Yilin Fan, Tobias Meyer
摘要

Contact inhibition of cell proliferation regulates tissue size and prevents uncontrolled cell expansion. When cell density increases, contact inhibition can force proliferating cells into quiescence. Here we show that the variable memory of local cell density experienced by a mother cell controls the levels of the cyclin-dependent kinase (CDK) activator cyclin D1 and inhibitor p27 in newborn daughters, which direct cells to proliferation or quiescence. Much of this regulation can be explained by rapid suppression of ERK activity by high cell density in mothers, which leads to lower cyclin D1 and higher p27 levels in daughters. Strikingly, cell density and mitogen signals compete by shifting the ratio of cyclin D1/p27 levels below or above a single sharp threshold that controls the proliferation decision. Thus, the history of competing cell density and mitogen signals experienced by mothers is funneled into a precise activator-inhibitor balance that decides the fate of daughter cells.

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Sigma-Aldrich
纤连蛋白牛血浆, solution, sterile-filtered, BioReagent, suitable for cell culture
Sigma-Aldrich
多西环素 单盐酸半乙醇半水合物