Nelson Institute of Environmental Medicine, New York University School of Medicine, Tuxedo, New York 10987, USA.
J Biol Chem. 2012 Apr 20;287(17):13752-60. doi: 10.1074/jbc.M111.337469. Epub 2012 Mar 5.
The Rho GDP dissociation inhibitor (RhoGDI) can bind to small GTPases and keep them in a biologically inactive state in cytoplasm, through which it affects actin polymerization and cell motility. However, mechanisms underlying how RhoGDI regulates Rho GTPase complex formation/membrane extraction/GTPase dissociation remain largely unexplored. Our previous studies reported that X-linked inhibitor of apoptosis protein (XIAP) interacted with RhoGDI via its RING domain and negatively modulated RhoGDI SUMOylation and HCT116 cancer cell migration. Here, we identified that RhoGDI SUMOylation specifically occurred at Lys-138, which was inhibited by XIAP domain. We further demonstrated that RhoGDI SUMOylation at Lys-138 was crucial for inhibiting actin polymerization and cytoskeleton formation as well as cancer cell motility. Moreover, SUMO-RhoGDI had a much higher binding affinity to small Rho GTPase compared with the un-SUMOylated form of RhoGDI. Taken together, our study demonstrated a novel modification of RhoGDI, SUMOylation at Lys-138, which played a key role in regulating Rho GTPase activation in cancer cells. The physiological regulation of RhoGDI SUMOylation by the RING domain of XIAP may account for modulation of cancer cell invasion and metastasis by XIAP.
Rho GDP 解离抑制剂 (RhoGDI) 可以通过其 RING 结构域与 RhoGDI 相互作用,并负向调节 RhoGDI 的 SUMO 化和 HCT116 癌细胞迁移。我们发现 RhoGDI 的 SUMO 化特异性发生在 Lys-138 上,这一过程受到 XIAP 结构域的抑制。我们进一步证明,RhoGDI 在 Lys-138 上的 SUMO 化对于抑制肌动蛋白聚合和细胞骨架形成以及癌细胞迁移至关重要。此外,SUMO-RhoGDI 与未 SUMO 化的 RhoGDI 形式相比,与小 Rho GTPase 的结合亲和力更高。综上所述,我们的研究表明 RhoGDI 的一种新型修饰形式,即 Lys-138 上的 SUMO 化,在调节癌细胞中 Rho GTP 酶的激活中发挥关键作用。XIAP 的 RING 结构域对 RhoGDI SUMO 化的生理调节可能解释了 XIAP 对癌细胞侵袭和转移的调节作用。
