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一种双稳态的Rb-E2F开关构成了限制点的基础。

A bistable Rb-E2F switch underlies the restriction point.

作者信息

Yao Guang, Lee Tae Jun, Mori Seiichi, Nevins Joseph R, You Lingchong

机构信息

Institute for Genome Sciences and Policy, Duke University, Durham, NC 27708, USA.

出版信息

Nat Cell Biol. 2008 Apr;10(4):476-82. doi: 10.1038/ncb1711. Epub 2008 Mar 23.

Abstract

The restriction point (R-point) marks the critical event when a mammalian cell commits to proliferation and becomes independent of growth stimulation. It is fundamental for normal differentiation and tissue homeostasis, and seems to be dysregulated in virtually all cancers. Although the R-point has been linked to various activities involved in the regulation of G1-S transition of the mammalian cell cycle, the underlying mechanism remains unclear. Using single-cell measurements, we show here that the Rb-E2F pathway functions as a bistable switch to convert graded serum inputs into all-or-none E2F responses. Once turned ON by sufficient serum stimulation, E2F can memorize and maintain this ON state independently of continuous serum stimulation. We further show that, at critical concentrations and duration of serum stimulation, bistable E2F activation correlates directly with the ability of a cell to traverse the R-point.

摘要

限制点(R点)标志着哺乳动物细胞开始增殖并变得独立于生长刺激的关键事件。它对于正常分化和组织稳态至关重要,并且在几乎所有癌症中似乎都失调。尽管R点与哺乳动物细胞周期G1-S转换调控中涉及的各种活动有关,但其潜在机制仍不清楚。通过单细胞测量,我们在此表明Rb-E2F途径作为一个双稳态开关,将分级的血清输入转化为全或无的E2F反应。一旦通过足够的血清刺激开启,E2F可以独立于持续的血清刺激而记忆并维持这种开启状态。我们进一步表明,在血清刺激的临界浓度和持续时间下,双稳态E2F激活与细胞穿越R点的能力直接相关。

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