Choi Shin Ae, Kim Steven J, Chung Kwang Chul
Department of Biology, College of Science, Yonsei University, Shinchon-dong 134, Seodaemun-gu, Seoul 120-749, Republic of Korea.
FEBS Lett. 2006 Oct 2;580(22):5275-82. doi: 10.1016/j.febslet.2006.08.076. Epub 2006 Sep 11.
Huntingtin interacting protein-1 (Hip1) is known to be associated with the N-terminal domain of huntingtin. Although Hip1 can induce apoptosis, the exact upstream signal transduction pathways have not been clarified yet. In the present study, we examined whether activation of intrinsic and/or extrinsic apoptotic pathways occurs during Hip1-mediated neuronal cell death. Overexpression of Hip1 induced cell death through caspase-3 activation in immortalized hippocampal neuroprogenitor cells. Interestingly, proteolytic processing of Hip1 into partial fragments was observed in response to Hip1 transfection and apoptosis-inducing drugs. Moreover, Hip1 was found to directly bind to and activate caspase-9. This promoted cytosolic release of cytochrome c and apoptosis-inducing factor via mitochondrial membrane perturbation. Furthermore, Hip1 could directly bind to Apaf-1, suggesting that the neurotoxic signals of Hip1 transmit through the intrinsic mitochondrial apoptotic pathways and the formation of apoptosome complex.
亨廷顿相互作用蛋白1(Hip1)已知与亨廷顿蛋白的N端结构域相关。尽管Hip1可诱导细胞凋亡,但其确切的上游信号转导通路尚未阐明。在本研究中,我们检测了在Hip1介导的神经元细胞死亡过程中,内源性和/或外源性凋亡通路是否被激活。在永生化海马神经祖细胞中,Hip1的过表达通过激活caspase-3诱导细胞死亡。有趣的是,在转染Hip1和凋亡诱导药物后,观察到Hip1被蛋白水解成部分片段。此外,发现Hip1可直接结合并激活caspase-9。这通过线粒体膜扰动促进了细胞色素c和凋亡诱导因子的胞质释放。此外,Hip1可直接结合Apaf-1,提示Hip1的神经毒性信号通过内源性线粒体凋亡通路和凋亡小体复合物的形成进行传递。
