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本文引用的文献

1
Cyclin-dependent kinase control of the initiation-to-elongation switch of RNA polymerase II.细胞周期蛋白依赖性激酶对 RNA 聚合酶 II 起始延伸转换的调控。
Nat Struct Mol Biol. 2012 Nov;19(11):1108-15. doi: 10.1038/nsmb.2399. Epub 2012 Oct 14.
2
Promoter-proximal pausing of RNA polymerase II: emerging roles in metazoans.RNA 聚合酶 II 的启动子近端暂停:后生动物中的新兴作用。
Nat Rev Genet. 2012 Oct;13(10):720-31. doi: 10.1038/nrg3293.
3
Cdk7: open questions beyond the prevailing model.细胞周期蛋白依赖性激酶7:主流模型之外的开放性问题。
Cell Cycle. 2012 Oct 1;11(19):3519-20. doi: 10.4161/cc.21888. Epub 2012 Aug 30.
4
Chemical genetics reveals a specific requirement for Cdk2 activity in the DNA damage response and identifies Nbs1 as a Cdk2 substrate in human cells.化学生物学揭示了 Cdk2 活性在 DNA 损伤反应中的特定需求,并确定 Nbs1 是人细胞中 Cdk2 的底物。
PLoS Genet. 2012 Aug;8(8):e1002935. doi: 10.1371/journal.pgen.1002935. Epub 2012 Aug 23.
5
A positive feedback loop links opposing functions of P-TEFb/Cdk9 and histone H2B ubiquitylation to regulate transcript elongation in fission yeast.正反馈环将 P-TEFb/Cdk9 和组蛋白 H2B 泛素化的相反功能联系起来,以调节裂殖酵母中转录延伸。
PLoS Genet. 2012;8(8):e1002822. doi: 10.1371/journal.pgen.1002822. Epub 2012 Aug 2.
6
Why minimal is not optimal: driving the mammalian cell cycle--and drug discovery--with a physiologic CDK control network.为什么最低限度不是最优的:利用生理 CDK 控制网络驱动哺乳动物细胞周期——和药物发现。
Cell Cycle. 2012 Jul 15;11(14):2600-5. doi: 10.4161/cc.20758.
7
Phosphorylation by cyclin-dependent kinase-9 controls ubiquitin-conjugating enzyme-2A function.周期蛋白依赖性激酶-9 的磷酸化控制泛素连接酶-2A 的功能。
Cell Cycle. 2012 Jun 1;11(11):2122-7. doi: 10.4161/cc.20548.
8
Serine-7 but not serine-5 phosphorylation primes RNA polymerase II CTD for P-TEFb recognition.丝氨酸-7而非丝氨酸-5的磷酸化使 RNA 聚合酶 II CTD 为 P-TEFb 识别做好准备。
Nat Commun. 2012 May 15;3:842. doi: 10.1038/ncomms1846.
9
Regulating the regulators: the pervasive effects of Pol II pausing on stimulus-responsive gene networks.调控调控因子:Pol II 暂停对刺激反应性基因网络的普遍影响。
Genes Dev. 2012 May 1;26(9):933-44. doi: 10.1101/gad.187781.112.
10
Separate domains of fission yeast Cdk9 (P-TEFb) are required for capping enzyme recruitment and primed (Ser7-phosphorylated) Rpb1 carboxyl-terminal domain substrate recognition.裂殖酵母 Cdk9(P-TEFb)的不同结构域对于帽酶的募集和被引物(Ser7 磷酸化)的 Rpb1 C 端结构域底物的识别是必需的。
Mol Cell Biol. 2012 Jul;32(13):2372-83. doi: 10.1128/MCB.06657-11. Epub 2012 Apr 16.

细胞周期蛋白依赖性激酶网络:连接细胞分裂周期与基因表达

The CDK Network: Linking Cycles of Cell Division and Gene Expression.

作者信息

Fisher Robert P

机构信息

Mount Sinai School of Medicine, New York, NY, USA.

出版信息

Genes Cancer. 2012 Nov;3(11-12):731-8. doi: 10.1177/1947601912473308.

DOI:10.1177/1947601912473308
PMID:23634260
原文链接:https://pmc.ncbi.nlm.nih.gov/articles/PMC3636752/
Abstract

Cyclin-dependent kinases (CDKs) play essential roles in cell proliferation and gene expression. Although distinct sets of CDKs work in cell division and transcription by RNA polymerase II (Pol II), they share a CDK-activating kinase (CAK), which is itself a CDK-Cdk7-in metazoans. Thus a unitary CDK network controls and may coordinate cycles of cell division and gene expression. Recent work reveals decisive roles for Cdk7 in both pathways. The CAK function of Cdk7 helps determine timing of activation and cyclin-binding preferences of different CDKs during the cell cycle. In the transcription cycle, Cdk7 is both an effector kinase, which phosphorylates Pol II and other proteins and helps establish promoter-proximal pausing; and a CAK for Cdk9 (P-TEFb), which releases Pol II from the pause. By governing the transition from initiation to elongation, Cdk7, Cdk9 and their substrates influence expression of genes important for developmental and cell-cycle decisions, and ensure co-transcriptional maturation of Pol II transcripts. Cdk7 engaged in transcription also appears to be regulated by phosphorylation within its own activation (T) loop. Here I review recent studies of CDK regulation in cell division and gene expression, and propose a model whereby mitogenic signals trigger a cascade of CDK T-loop phosphorylation that drives cells past the restriction (R) point, when continued cell-cycle progression becomes growth factor-independent. Because R-point control is frequently deregulated in cancer, the CAK-CDK pathway is an attractive target for chemical inhibition aimed at impeding the inappropriate commitment to cell division.

摘要

细胞周期蛋白依赖性激酶(CDKs)在细胞增殖和基因表达中发挥着至关重要的作用。尽管不同组的CDKs在细胞分裂以及RNA聚合酶II(Pol II)介导的转录过程中发挥作用,但它们共享一种CDK激活激酶(CAK),在多细胞动物中该激酶本身是一种CDK - Cdk7。因此,一个统一的CDK网络控制并可能协调细胞分裂和基因表达的周期。最近的研究揭示了Cdk7在这两个途径中都起着决定性作用。Cdk7的CAK功能有助于确定细胞周期中不同CDKs的激活时间和细胞周期蛋白结合偏好。在转录周期中,Cdk7既是一种效应激酶,可磷酸化Pol II和其他蛋白质并有助于建立启动子近端暂停;也是Cdk9(P - TEFb)的CAK,可使Pol II从暂停状态释放。通过控制从起始到延伸的转变,Cdk7、Cdk9及其底物影响对发育和细胞周期决策至关重要的基因的表达,并确保Pol II转录本的共转录成熟。参与转录的Cdk7似乎也受到其自身激活(T)环内磷酸化的调节。在此,我回顾了近期关于细胞分裂和基因表达中CDK调节的研究,并提出了一个模型,即促有丝分裂信号触发一系列CDK T环磷酸化,从而驱动细胞越过限制(R)点,此时细胞周期的持续进展变得不依赖生长因子。由于R点控制在癌症中经常失调,CAK - CDK途径是旨在阻止不适当的细胞分裂承诺的化学抑制的一个有吸引力的靶点。