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Selective ablation of retinoblastoma protein function by the RET finger protein

机译:RET指状蛋白选择性切除视网膜母细胞瘤蛋白功能

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摘要

The retinoblastoma tumor suppressor protein (Rb) affects gene transcription both negatively and positively and through this regulates distinct cellular responses. Although cell cycle regulation requires gene repression, Rb's ability to promote differentiation and part of its anti proliferative activity appears to rely on the activation of gene transcription. We present evidence here that the RET finger protein (RFP)/tripartite motif protein 27 (TRIM 27) inhibits gene transcription activation by Rb but does not affect gene repression. RFP binds to Rb and prevents the degradation of the EID-1 inhibitor of histone acetylation and differentiation. Furthermore, ablation of RFP in U2OS osteosarcoma cells augments a transcriptional program indicative of lineage-specific differentiation in response to Rb. These findings provide precedent for a regulatory pathway that uncouples different Rb-dependent activities and thus silences specific cellular responses to Rb in a selective way.
机译:视网膜母细胞瘤抑癌蛋白(Rb)对基因转录产生负面和正面影响,并由此调节不同的细胞反应。尽管细胞周期调节需要基因抑制,但Rb促进分化的能力及其部分抗增殖活性似乎依赖于基因转录的激活。我们在这里提供证据,RET手指蛋白(RFP)/三方基序蛋白27(TRIM 27)抑制Rb的基因转录激活,但不影响基因抑制。 RFP与Rb结合并阻止EID-1抑制剂对组蛋白乙酰化和分化的降解。此外,U2OS骨肉瘤细胞中RFP的消融增强了转录程序,该程序指示了对Rb的谱系特异性分化。这些发现为调节途径打开了先例,该调节途径使不同的Rb依赖性活动脱钩,从而以选择性的方式沉默了对Rb的特定细胞应答。

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