Wooten Marie W, Geetha Thangiah, Seibenhener M Lamar, Babu J Ramesh, Diaz-Meco Maria T, Moscat Jorge
Department of Biological Sciences, Program in Cell and Molecular Biosciences, Auburn University, Alabama 36849, USA.
J Biol Chem. 2005 Oct 21;280(42):35625-9. doi: 10.1074/jbc.C500237200. Epub 2005 Aug 3.
Sequestosome 1/p62 is a scaffolding protein with several interaction modules that include a PB1 dimerization domain, a TRAF6 (tumor necrosis factor receptor-associated factor 6) binding site, and a ubiquitin-associating (UBA) domain. Here, we report that p62 functions to facilitate K63-polyubiquitination of TRAF6 and thereby mediates nerve growth factor-induced activation of the NF-kappaB pathway. In brain of p62 knock-out mice we did not recover polyubiquitinated TRAF6. The UBA domain binds polyubiquitin chains and deletion of p62-UBA domain or mutation of F406V within the ubiquitin binding pocket of the UBA domain abolished TRAF6 polyubiquitination. Likewise, deletion of p62 N-terminal dimerization domain or the TRAF6 binding site had similar effects on both polyubiquitination and oligomerization of TRAF6. Nerve growth factor treatment of PC12 cells induced TRAF6 polyubiquitination along with formation of a p62-TRAF6-IKKbeta-PKC iota signal complex, while inhibition of the p62/TRAF6 interaction had an opposite effect. These results provide evidence for a mechanism whereby p62 serves to regulate the NF-kappaB pathway.
聚集体蛋白1/p62是一种具有多个相互作用模块的支架蛋白,这些模块包括一个PB1二聚化结构域、一个TRAF6(肿瘤坏死因子受体相关因子6)结合位点和一个泛素结合(UBA)结构域。在此,我们报告p62的功能是促进TRAF6的K63-多聚泛素化,从而介导神经生长因子诱导的NF-κB信号通路的激活。在p62基因敲除小鼠的大脑中,我们未检测到多聚泛素化的TRAF6。UBA结构域结合多聚泛素链,p62-UBA结构域的缺失或UBA结构域泛素结合口袋内F406V的突变消除了TRAF6的多聚泛素化。同样,p62 N端二聚化结构域或TRAF6结合位点的缺失对TRAF6的多聚泛素化和寡聚化也有类似影响。神经生长因子处理PC12细胞可诱导TRAF6多聚泛素化,并形成p62-TRAF6-IKKβ-PKC ι信号复合物,而抑制p62/TRAF6相互作用则产生相反的效果。这些结果为p62调控NF-κB信号通路的机制提供了证据。
