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F-box蛋白底物的鉴定。

Identification of substrates for F-box proteins.

作者信息

Jin Jianping, Ang Xiaolu L, Shirogane Takahiro, Wade Harper J

机构信息

Department of Pathology, Harvard Medical School, Boston, Massachusetts, USA.

出版信息

Methods Enzymol. 2005;399:287-309. doi: 10.1016/S0076-6879(05)99020-4.

DOI:10.1016/S0076-6879(05)99020-4
PMID:16338364
Abstract

F-box proteins serve as specificity factors for a family of ubiquitin protein ligases composed of Skp1, Cu11, and Rbx1. In SCF complexes, Cu11 serves as a scaffold for assembly of the catalytic components composed of Rbx1 and a ubiquitin-conjugating enzyme and the specificity module composed of Skp1 and an F-box protein. F-box proteins interact with Skp1 through the F-box motif and with ubiquitination substrates through C-terminal protein interaction domains such as WD40 repeats. The human genome contains approximately 68 F-box proteins, which fall into three major classes: Fbws containing WD40 repeats, Fbls containing leucine-rich repeats, and Fbxs containing other types of domains. Most often, F-box proteins interact with their targets in a phosphorylation-dependent manner. The interaction of F-box proteins with substrates typically involves a phosphodegron, a small peptide motif containing specific phosphorylation events whose sequence is complementary to the F-box protein. The identification of substrates of F-box proteins is frequently a challenge because of the relatively weak affinity of substrates for the requisite F-box protein. Here we describe approaches for the identification of substrates of F-box proteins. Approaches include stabilization of ubiquitination targets by Cu11-dominant negatives, the use of shRNA hairpins to disrupt F-box protein expression, and the use of collections of F-box proteins as biochemical reagents to identify interacting proteins that may be substrates. In addition, we describe approaches for the use of immobilized phosphopeptides to identify F-box proteins that recognize particular phosphodegrons.

摘要

F-box蛋白作为一类泛素蛋白连接酶的特异性因子,这类连接酶由Skp1、Cul1和Rbx1组成。在SCF复合物中,Cul1作为一个支架,用于组装由Rbx1和泛素结合酶组成的催化组分以及由Skp1和一个F-box蛋白组成的特异性模块。F-box蛋白通过F-box基序与Skp1相互作用,并通过C端蛋白相互作用结构域(如WD40重复序列)与泛素化底物相互作用。人类基因组包含大约68种F-box蛋白,它们可分为三大类:含有WD40重复序列的Fbws、含有富含亮氨酸重复序列的Fbls以及含有其他类型结构域的Fbxs。大多数情况下,F-box蛋白以磷酸化依赖的方式与其靶标相互作用。F-box蛋白与底物的相互作用通常涉及一个磷酸化降解基序,这是一个包含特定磷酸化事件的小肽基序,其序列与F-box蛋白互补。由于底物对所需F-box蛋白的亲和力相对较弱,鉴定F-box蛋白的底物常常是一项挑战。在此,我们描述了鉴定F-box蛋白底物的方法。这些方法包括通过Cul1显性负突变体稳定泛素化靶标、使用shRNA发夹结构破坏F-box蛋白表达,以及使用F-box蛋白集合作为生化试剂来鉴定可能作为底物的相互作用蛋白。此外,我们还描述了使用固定化磷酸肽来鉴定识别特定磷酸化降解基序的F-box蛋白的方法

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