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CAMP-mediated inhibition of DNA replication and S phase progression: Involvement of Rb, p21(Cip1), and PCNA

机译:CAMP介导的DNA复制和S期进程的抑制:Rb,p21(Cip1)和PCNA的参与。

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cAMP exerts an antiproliferative effect on a number of cell types including lymphocytes. This effect of cAMP is proposed to be mediated by its ability to inhibit G1/S transition. In this report, we provide evidence for a new mechanism whereby cAMP might inhibit cellular proliferation. We show that elevation of intracellular levels of cAMP inhibits DNA replication and arrests the cells in S phase. The cAMP-induced inhibition of DNA synthesis was associated with the increased binding of p21(cip1) to Cdk2-cyclin complexes, inhibition of Cdk2 kinase activity, dephosphorylation of Rb, and dissociation of PCNA from chromatin in S phase cells. The ability of cAMP to inhibit DNA replication and trigger release of PCNA from chromatin required Rb and p21(Cip1) proteins, since both processes were only marginally affected by increased levels of cAMP in Rb-/- and p21(Cip1-/-) 3T3 fibroblasts. Importantly, the implications of cAMP-induced inhibition of DNA synthesis in cancer treatment was demonstrated by the ability of cAMP to reduce apoptosis induced by S phase-specific cytotoxic drugs. Taken together, these results demonstrate a novel role for cAMP in regulation of DNA synthesis and support a model in which activation of cAMP-dependent signaling protects cells from the effect of S phase-specific antitumor agents.
机译:cAMP对包括淋巴细胞在内的多种细胞类型具有抗增殖作用。有人认为,cAMP的这种作用是由其抑制G1 / S转变的能力介导的。在本报告中,我们为cAMP可能抑制细胞增殖的新机制提供了证据。我们表明,细胞内cAMP水平的升高会抑制DNA复制并使S期细胞停滞。 cAMP诱导的DNA合成抑制与p21(cip1)与Cdk2-cyclin复合物的结合增加,Cdk2激酶活性的抑制,Rb的去磷酸化以及PCNA从S期细胞中的染色质解离有关。 cAMP抑制DNA复制并触发PCNA从染色质释放的能力需要Rb和p21(Cip1)蛋白,因为这两个过程仅受Rb-/-和p21(Cip1-/-)3T3中cAMP水平升高的轻微影响成纤维细胞。重要的是,cAMP减少S期特异性细胞毒性药物诱导的凋亡的能力证明了cAMP诱导的DNA合成抑制在癌症治疗中的意义。综上所述,这些结果证明了cAMP在调节DNA合成中的新作用,并支持其中cAMP依赖性信号转导保护细胞免受S期特异性抗肿瘤剂影响的模型。

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