Kim Hyoung Tae, Kim Kwang Pyo, Uchiki Tomoaki, Gygi Steven P, Goldberg Alfred L
Department of Cell Biology, Harvard Medical School, Boston, MA 02115, USA.
EMBO J. 2009 Jul 8;28(13):1867-77. doi: 10.1038/emboj.2009.115. Epub 2009 Apr 23.
Ubiquitin (Ub)-protein conjugates formed by purified ring-finger or U-box E3s with the E2, UbcH5, resist degradation and disassembly by 26S proteasomes. These chains contain multiple types of Ub forks in which two Ub's are linked to adjacent lysines on the proximal Ub. We tested whether cells contain factors that prevent formation of nondegradable conjugates and whether the forked chains prevent proteasomal degradation. S5a is a ubiquitin interacting motif (UIM) protein present in the cytosol and in the 26S proteasome. Addition of S5a or a GST-fusion of S5a's UIM domains to a ubiquitination reaction containing 26S proteasomes, UbcH5, an E3 (MuRF1 or CHIP), and a protein substrate, dramatically stimulated its degradation, provided S5a was present during ubiquitination. Mass spectrometry showed that S5a and GST-UIM prevented the formation of Ub forks without affecting synthesis of standard isopeptide linkages. The forked Ub chains bind poorly to 26S proteasomes unlike those synthesized with S5a present or linked to Lys63 or Lys48 chains. Thus, S5a (and presumably certain other UIM proteins) function with certain E3/E2 pairs to ensure synthesis of efficiently degraded non-forked Ub conjugates.
由纯化的具有E2(UbcH5)的指环结构域或U-box E3形成的泛素(Ub)-蛋白缀合物可抵抗26S蛋白酶体的降解和拆解。这些链包含多种类型的Ub叉,其中两个Ub与近端Ub上相邻的赖氨酸相连。我们测试了细胞中是否含有阻止形成不可降解缀合物的因子,以及叉状链是否会阻止蛋白酶体降解。S5a是一种存在于细胞质和26S蛋白酶体中的泛素相互作用基序(UIM)蛋白。在含有26S蛋白酶体、UbcH5、一种E3(MuRF1或CHIP)和一种蛋白质底物的泛素化反应中添加S5a或S5a的UIM结构域的GST融合蛋白,可显著刺激其降解,前提是在泛素化过程中存在S5a。质谱分析表明,S5a和GST-UIM可阻止Ub叉的形成,而不影响标准异肽键的合成。与在有S5a存在的情况下合成的或与Lys63或Lys48链相连的Ub链不同,叉状Ub链与26S蛋白酶体的结合较差。因此,S5a(可能还有某些其他UIM蛋白)与某些E3/E2对共同作用,以确保合成可有效降解的非叉状Ub缀合物。
