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NIRF/UHRF2 在细胞周期网络中占据中心位置,并允许与表观遗传景观相耦合。

NIRF/UHRF2 occupies a central position in the cell cycle network and allows coupling with the epigenetic landscape.

机构信息

Department of Human Lifesciences, Fukushima Medical University School of Nursing, Fukushima, Japan.

出版信息

FEBS Lett. 2012 Jun 4;586(11):1570-83. doi: 10.1016/j.febslet.2012.04.038. Epub 2012 Apr 30.

Abstract

As predicted by systems biology, a paradigm shift will emerge through the integration of information about different layers of cellular processes. The cell cycle network is at the heart of the cellular computing system, and orchestrates versatile cellular functions. The NIRF/UHRF2 ubiquitin ligase is an "intermodular hub" that occupies a central position in the network, and facilitates coordination among the cell cycle machinery, the ubiquitin-proteasome system, and the epigenetic system. NIRF interacts with cyclins, CDKs, p53, pRB, PCNA, HDAC1, DNMTs, G9a, methylated histone H3 lysine 9, and methylated DNA. NIRF ubiquitinates cyclins D1 and E1, and induces G1 arrest. The NIRF gene is frequently lost in tumors and is a candidate tumor suppressor, while its paralog, the UHRF1 gene, is hardly altered. Thus, investigations of NIRF are essential to understand the entire biological systems. Through integration of the enormous information flows, NIRF may contribute to the coupling between the cell cycle network and the epigenetic landscape. We propose the new paradigm that NIRF produces the extreme diversity in the network wiring that helps the diversity of Waddington's canals.

摘要

正如系统生物学所预测的那样,通过整合不同细胞过程层面的信息,将出现范式转变。细胞周期网络是细胞计算系统的核心,它协调着多种细胞功能。NIRF/UHRF2 泛素连接酶是一个“模块间枢纽”,在网络中占据中心位置,促进细胞周期机制、泛素-蛋白酶体系统和表观遗传系统之间的协调。NIRF 与细胞周期蛋白、CDK、p53、pRB、PCNA、HDAC1、DNMTs、G9a、组蛋白 H3 赖氨酸 9 甲基化和甲基化 DNA 相互作用。NIRF 泛素化细胞周期蛋白 D1 和 E1,并诱导 G1 期停滞。NIRF 基因在肿瘤中经常缺失,是候选肿瘤抑制基因,而其同源基因 UHRF1 基因几乎没有改变。因此,对 NIRF 的研究对于理解整个生物系统至关重要。通过整合巨大的信息流,NIRF 可能有助于细胞周期网络和表观遗传景观之间的耦合。我们提出了一个新的范式,即 NIRF 产生了网络布线的极端多样性,有助于 Waddington 运河的多样性。

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