Department of Biology, College of Science, Illinois Institute of Technology, Chicago, IL, 60616, USA.
Department of Biology, College of Science, Illinois Institute of Technology, Chicago, IL, 60616, USA.
Biochem Biophys Res Commun. 2018 Sep 18;503(4):3192-3197. doi: 10.1016/j.bbrc.2018.08.123. Epub 2018 Aug 24.
Ubl4A is a small ubiquitin-like protein involved in diverse cellular functions. We have shown that Ubl4A is critical for survival of the starvation-mediated cell death in vivo. The underlying mechanism for this is through interaction with the actin-related protein Arp2/3 complex and promotion of actin branching. Interestingly, "put-back" of Ubl4A to Ubl4A-deficient cells also results in cell death. Removal of the Ubl4A N-terminus significantly enhances its cytotoxicity, indicating that the pro-death activity of Ubl4A is mainly from its C-terminal region. In vitro protein pull-down assays show that the C-terminal region of Ubl4A can directly interact with the Arp2/3 complex. The single point mutation of an aspartic acid to alanine (D122A) in the Ubl4A C-terminus abolishes its ability to bind the Arp2/3 complex. This mutation also destabilizes Ubl4A proteins susceptible to protease degradation. Importantly, ectopic expression of wild-type Ubl4A can induce cell death in colon cancer cells, but such pro-death activity is diminished in the D122A mutant. These data suggest that Ubl4A C-terminus, especially D122, is critical for Ubl4A-Arp2/3 interaction and its pro-death function.
Ubl4A 是一种参与多种细胞功能的小泛素样蛋白。我们已经表明,Ubl4A 对于体内饥饿介导的细胞死亡的存活至关重要。其潜在机制是通过与肌动蛋白相关蛋白 Arp2/3 复合物相互作用并促进肌动蛋白分支。有趣的是,将 Ubl4A“放回” Ubl4A 缺陷细胞也会导致细胞死亡。去除 Ubl4A 的 N 端显著增强了其细胞毒性,表明 Ubl4A 的促死亡活性主要来自其 C 端区域。体外蛋白下拉实验表明,Ubl4A 的 C 端区域可以直接与 Arp2/3 复合物相互作用。Ubl4A C 端的一个天冬氨酸突变为丙氨酸(D122A)会使其丧失与 Arp2/3 复合物结合的能力。这种突变还会使 Ubl4A 蛋白不稳定,容易被蛋白酶降解。重要的是,外源性表达野生型 Ubl4A 可诱导结肠癌细胞死亡,但在 D122A 突变体中,这种促死亡活性降低。这些数据表明,Ubl4A 的 C 端,特别是 D122,对于 Ubl4A-Arp2/3 相互作用及其促死亡功能至关重要。
