Neuroscience Graduate Group.
Vanderbilt Brain Institute.
J Neurosci. 2018 Aug 1;38(31):6825-6840. doi: 10.1523/JNEUROSCI.0699-18.2018. Epub 2018 Jun 22.
The C terminus of HSC70-interacting protein (CHIP, ) is a ubiquitously expressed cytosolic E3-ubiquitin ligase. CHIP-deficient mice exhibit cardiovascular stress and motor dysfunction before premature death. This phenotype is more consistent with animal models in which master regulators of autophagy are affected rather than with the mild phenotype of classic E3-ubiquitin ligase mutants. The cellular and biochemical events that contribute to neurodegeneration and premature aging in CHIP KO models remain poorly understood. Electron and fluorescent microscopy demonstrates that CHIP deficiency is associated with greater numbers of mitochondria, but these organelles are swollen and misshapen. Acute bioenergetic stress triggers CHIP induction and relocalization to mitochondria, where it plays a role in the removal of damaged organelles. This mitochondrial clearance is required for protection following low-level bioenergetic stress in neurons. CHIP expression overlaps with stabilization of the redox stress sensor PTEN-inducible kinase 1 (PINK1) and is associated with increased LC3-mediated mitophagy. Introducing human promoter-driven vectors with mutations in either the E3 ligase or tetracopeptide repeat domains of CHIP in primary neurons derived from CHIP-null animals enhances CHIP accumulation at mitochondria. Exposure to autophagy inhibitors suggests that the increase in mitochondrial CHIP is likely due to diminished clearance of these CHIP-tagged organelles. Proteomic analysis of WT and CHIP KO mouse brains (four male, four female per genotype) reveals proteins essential for maintaining energetic, redox, and mitochondrial homeostasis undergo significant genotype-dependent expression changes. Together, these data support the use of CHIP-deficient animals as a predictive model of age-related degeneration with selective neuronal proteotoxicity and mitochondrial failure. Mitochondria are recognized as central determinants of neuronal function and survival. We demonstrate that C terminus of HSC70-Interacting Protein (CHIP) is critical for neuronal responses to stress. CHIP upregulation and localization to mitochondria is required for mitochondrial autophagy (mitophagy). Unlike other disease-associated E3 ligases such as Parkin and Mahogunin, CHIP controls homeostatic and stress-induced removal of mitochondria. Although CHIP deletion results in greater numbers of mitochondria, these organelles have distorted inner membranes without clear cristae. Neuronal cultures derived from animals lacking CHIP are more vulnerable to acute injuries and transient loss of CHIP renders neurons incapable of mounting a protective response after low-level stress. Together, these data suggest that CHIP is an essential regulator of mitochondrial number, cell signaling, and survival.
HSC70 相互作用蛋白 (CHIP) 的 C 端是一种广泛表达的胞质 E3-泛素连接酶。CHIP 缺陷小鼠在过早死亡前表现出心血管应激和运动功能障碍。这种表型与自噬的主要调节剂受到影响的动物模型更为一致,而与经典 E3-泛素连接酶突变体的轻度表型不一致。导致 CHIP KO 模型中神经退行性变和早衰的细胞和生化事件仍知之甚少。电子和荧光显微镜表明,CHIP 缺乏与更多数量的线粒体有关,但这些细胞器肿胀变形。急性生物能量应激触发 CHIP 诱导和重定位到线粒体,在那里它在清除受损细胞器中发挥作用。神经元中低水平生物能量应激后的保护需要这种线粒体清除。CHIP 表达与氧化还原应激传感器 PTEN 诱导激酶 1 (PINK1) 的稳定重叠,并与增加的 LC3 介导的线粒体自噬有关。在源自 CHIP 缺失动物的原代神经元中引入具有 CHIP 的 E3 连接酶或四肽重复结构域突变的人启动子驱动载体,可增强线粒体中 CHIP 的积累。自噬抑制剂的暴露表明,线粒体 CHIP 的增加可能是由于这些 CHIP 标记细胞器的清除减少所致。WT 和 CHIP KO 小鼠大脑的蛋白质组分析(每种基因型 4 只雄性,4 只雌性)显示,维持能量、氧化还原和线粒体动态平衡的蛋白质发生显著的基因型依赖性表达变化。这些数据共同支持使用 CHIP 缺陷动物作为具有选择性神经元蛋白毒性和线粒体衰竭的与年龄相关退化的预测模型。线粒体被认为是神经元功能和存活的核心决定因素。我们证明 C 端的热休克蛋白 70 相互作用蛋白 (CHIP) 对神经元应激反应至关重要。CHIP 的上调和向线粒体的定位对于线粒体自噬(mitophagy)是必需的。与其他疾病相关的 E3 连接酶,如 Parkin 和 Mahogunin 不同,CHIP 控制着线粒体的稳态和应激诱导的清除。尽管 CHIP 缺失导致更多数量的线粒体,但这些细胞器的内膜扭曲,没有明显的嵴。缺乏 CHIP 的动物衍生的神经元培养物对急性损伤更敏感,并且 CHIP 的瞬时缺失使得神经元在低水平应激后无法产生保护反应。这些数据表明,CHIP 是线粒体数量、细胞信号和存活的必需调节剂。
