Department of Molecular Medicine, Institute of Biotechnology, University of Texas Health Science Center, San Antonio, TX 78245, USA.
Proc Natl Acad Sci U S A. 2011 Aug 16;108(33):13558-63. doi: 10.1073/pnas.1104051108. Epub 2011 Aug 1.
Rad23 and cell division cycle protein 48 (Cdc48), two key regulators of postubiquitylation events, act on distinct and overlapping sets of substrates. The principle underlying their division of labor and cooperation in proteolysis remains elusive. Both Rad23 and Cdc48 bind a ubiquitin protein ligase ubiquitin fusion degradation-2 (Ufd2), and regulate the degradation of Ufd2 substrates. With its ability to bind ubiquitin chains directly and the proteasome via different domains, Rad23 serves as a bridge linking ubiquitylated substrates to the proteasome. The significance and specific role of the Ufd2-Cdc48 interaction are unclear. Here, we demonstrate that mutations in Ufd2 alter its interaction with Cdc48 and impair its function in substrate proteolysis but not in ubiquitylation. Furthermore, Cdc48 promotes the disassembly of the Ufd2-Rad23 complex in an manner that is dependent on ATP and Ufd2 binding, revealing a biochemical role for Cdc48. Rad23 was shown to bind separately to Ufd2 and to the proteasome subunit Rpn1, which define two distinct steps in proteolysis. The action of Cdc48 could free Rad23 from Ufd2 to allow its subsequent association with Rpn1, which in turn may facilitate the orderly transfer of the substrate from the ubiquitylation apparatus to the proteasome.
Rad23 和细胞分裂周期蛋白 48(Cdc48)是泛素化后事件的两个关键调节因子,它们作用于不同且重叠的底物集合。它们在蛋白酶体降解中分工与合作的基本原则仍然难以捉摸。Rad23 和 Cdc48 都与泛素蛋白连接酶 ubiquitin fusion degradation-2(Ufd2)结合,并调节 Ufd2 底物的降解。Rad23 通过不同的结构域直接结合泛素链和蛋白酶体,充当将泛素化底物连接到蛋白酶体的桥梁。Ufd2-Cdc48 相互作用的意义和特定作用尚不清楚。在这里,我们证明 Ufd2 中的突变改变了其与 Cdc48 的相互作用,并损害了其在底物蛋白酶体降解中的功能,但不影响泛素化。此外,Cdc48 以依赖于 ATP 和 Ufd2 结合的方式促进 Ufd2-Rad23 复合物的解体,揭示了 Cdc48 的生化作用。Rad23 被证明分别与 Ufd2 和蛋白酶体亚基 Rpn1 结合,这定义了蛋白酶体降解中的两个不同步骤。Cdc48 的作用可以使 Rad23 从 Ufd2 上释放出来,从而允许其随后与 Rpn1 结合,这反过来又可能促进底物从泛素化装置到蛋白酶体的有序转移。
