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Network calisthenics: control of E2F dynamics in cell cycle entry.

机译:网络健美操:控制细胞周期进入过程中的E2F动态。

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Stimulation of quiescent mammalian cells with mitogens induces an abrupt increase in E2F1-3 expression just prior to the onset of DNA synthesis, followed by a rapid decline as replication ceases. This temporal adaptation in E2F facilitates a transient pattern of gene expression that reflects the ordered nature of DNA replication. The challenge to understand how E2F dynamics coordinate molecular events required for high-fidelity DNA replication has great biological implications. Indeed, precocious, prolonged, elevated or reduced accumulation of E2F can generate replication stress that culminates in either arrest or death. Accordingly, temporal characteristics of E2F are regulated by several network modules that include feedforward and autoregulatory loops. In this review, we discuss how these network modules contribute to "shaping" E2F dynamics in the context of mammalian cell cycle entry.
机译:就在DNA合成开始之前,用促分裂原刺激静止的哺乳动物细胞会引起E2F1-3表达的突然增加,然后随着复制的停止而迅速下降。 E2F中的这种时间适应性促进了基因表达的瞬时模式,反映了DNA复制的有序性质。理解E2F动力学如何协调高保真DNA复制所需的分子事件的挑战具有重大的生物学意义。确实,过早,长时间,升高或降低的E2F积累会产生复制压力,最终导致逮捕或死亡。因此,E2F的时间特性由包括前馈和自动调节回路在内的几个网络模块调节。在这篇综述中,我们讨论了这些网络模块如何在哺乳动物细胞周期进入的背景下促进“塑造” E2F动态。

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