The nuclear localization of SET mediated by impalpha3/impbeta attenuates its cytosolic toxicity in neurons |
| |
Authors: | Qu Dianbo Zhang Yi Ma Jing Guo Ke Li Rong Yin Yijun Cao Xinmin Park David S |
| |
Institution: | Institute of Molecular and Cell Biology, Proteos, Singapore, Singapore. dqu@uottawa.ca |
| |
Abstract: | SET is a multi-functional protein in proliferating cells. Some of the proposed functions of SET suggest an important nuclear role. However, the nuclear import pathway of SET is also unknown and the function of SET in neurons is unclear. Presently, using cortical neurons, we report that the nuclear import of SET is mediated by an impalpha/impbeta-dependent pathway. Nuclear localization signal, (168)KRSSQTQNKASRKR(181), in SET interacts with impalpha3, which recruits impbeta to form a ternary complex, resulting in efficient transportation of SET into nucleus. By in vitro nuclear import assay based on digitonin-permeabilized neurons, we further demonstrated that the nuclear import of SET relies on Ran GTPase. We provide evidence that this nuclear localization of SET is important in neuronal survival. Under basal conditions, SET is predominately nuclear. However, upon death induced by genotoxic stress, endogenous SET decreases in the nucleus and increases in the cytoplasm. Consistent with a toxic role of SET in the cytoplasm, targeted expression of SET to the cytoplasm exacerbates death compared to wild type SET expression which is protective following DNA damage. Taken together, our results indicate that SET is imported into the nucleus through its association with impalpha3/impbeta, and that localization of SET is important in regulation of neuronal death. |
| |
Keywords: | cell death importin nuclear import SET protein |
本文献已被 PubMed 等数据库收录! |
|