Yao Tingting, Song Ling, Jin Jingji, Cai Yong, Takahashi Hidehisa, Swanson Selene K, Washburn Michael P, Florens Laurence, Conaway Ronald C, Cohen Robert E, Conaway Joan W
Stowers Institute for Medical Research, Kansas City, MO 64110, USA.
Mol Cell. 2008 Sep 26;31(6):909-17. doi: 10.1016/j.molcel.2008.08.027.
Deubiquitinating enzymes (DUBs) are proteases that can antagonize ubiquitin-mediated signaling by disassembling ubiquitin-protein conjugates. How DUBs are regulated in vivo and how their substrate specificities are achieved are largely unknown. The conserved DUB Uch37 is found on proteasomes in organisms ranging from fission yeast to humans. Deubiquitination by Uch37 is activated by proteasomal binding, which enables Uch37 to process polyubiquitin chains. Here we show that in the nucleus Uch37 is also associated with the human Ino80 chromatin-remodeling complex (hINO80). In hINO80, Uch37 is held in an inactive state; however, it can be activated by transient interaction of the Ino80 complex with the proteasome. Thus, DUB activities can be modulated both positively and negatively via dynamic interactions with partner proteins. In addition, our findings suggest that the proteasome and the hINO80 chromatin-remodeling complex may cooperate to regulate transcription or DNA repair, processes in which both complexes have been implicated.
去泛素化酶(DUBs)是一类蛋白酶,能够通过拆解泛素-蛋白质缀合物来拮抗泛素介导的信号传导。DUBs在体内如何被调控以及它们的底物特异性是如何实现的,目前仍知之甚少。保守的DUB Uch37存在于从裂殖酵母到人类等多种生物的蛋白酶体上。Uch37的去泛素化作用通过蛋白酶体结合而被激活,这使得Uch37能够处理多聚泛素链。在此,我们表明在细胞核中,Uch37还与人类Ino80染色质重塑复合体(hINO80)相关联。在hINO80中,Uch37处于无活性状态;然而,它可以通过Ino80复合体与蛋白酶体的短暂相互作用而被激活。因此,DUB的活性可以通过与伴侣蛋白的动态相互作用而得到正向和负向的调节。此外,我们的研究结果表明,蛋白酶体和hINO80染色质重塑复合体可能协同调节转录或DNA修复,而这两个复合体均与这些过程有关。