Abida Wassim M, Nikolaev Anatoly, Zhao Wenhui, Zhang Wenzhu, Gu Wei
Institute for Cancer Genetics and the Department of Pathology, College of Physicians & Surgeons, Columbia University, New York, New York 10032, USA.
J Biol Chem. 2007 Jan 19;282(3):1797-804. doi: 10.1074/jbc.M609001200. Epub 2006 Nov 9.
The p53 tumor suppressor is regulated by post-translational modification, including ubiquitination, phosphorylation and acetylation. It has previously been shown that the ubiquitin ligase Mdm2 also promotes the conjugation of Nedd8, a ubiquitin-like protein, to p53, inhibiting its transcriptional activity. We report the identification of FBXO11, a member of the F-box protein family and a component of the Skp1.Cullin1.F-box (SCF) complex, as a new p53-interacting protein. We show that FBXO11 promotes the neddylation of p53 both in vitro and in vivo. In addition to the C-terminal lysine residues, FBXO11 can also promote Nedd8 conjugation to Lys-320 and Lys-321, and neddylation of p53 leads to suppression of p53 function. This is consistent with recent studies showing that a lysine to arginine mutation at Lys-320 significantly enhances p53 function, although Lys-320 was originally identified as an acetylation site involving PCAF-mediated activation of p53. Our study provides an example of an F-box protein acting as an adaptor protein that can mediate the neddylation of a non-cullin substrate.
p53肿瘤抑制蛋白受翻译后修饰调控,包括泛素化、磷酸化和乙酰化。此前已有研究表明,泛素连接酶Mdm2还能促进类泛素蛋白Nedd8与p53结合,抑制其转录活性。我们报告了F-box蛋白家族成员、Skp1.Cullin1.F-box(SCF)复合体的组成部分FBXO11作为一种新的与p53相互作用的蛋白的鉴定结果。我们发现FBXO11在体外和体内均能促进p53的Nedd8化。除了C末端赖氨酸残基外,FBXO11还能促进Nedd8与赖氨酸320和赖氨酸321结合,而p53的Nedd8化会导致p53功能受到抑制。这与最近的研究结果一致,即赖氨酸320处的赖氨酸到精氨酸突变显著增强了p53功能,尽管赖氨酸320最初被鉴定为涉及PCAF介导的p53激活的乙酰化位点。我们的研究提供了一个F-box蛋白作为衔接蛋白介导非Cullin底物Nedd8化的例子。
