Functional genomics laboratory, Center for Medical Engineering, SBST Vellore Institute of Technology, Vellore, TN, India.
J Neurochem. 2012 Feb;120(3):350-70. doi: 10.1111/j.1471-4159.2011.07588.x. Epub 2011 Dec 21.
The study of neurodegenerative disorders has had a major impact on our understanding of more fundamental mechanisms underlying neurobiology. Breakthroughs in the genetics of Alzheimer's (AD) and Parkinson's diseases (PD) has resulted in new knowledge in the areas of axonal transport, energy metabolism, protein trafficking/clearance and synaptic physiology. The major neurodegenerative diseases have in common a regional or network pathology associated with abnormal protein accumulation(s) and various degrees of motor or cognitive decline. In AD, β-amyloids are deposited in extracellular diffuse and compacted plaques as well as intracellularly. There is a major contribution to the disease by the co-existence of an intraneuronal tauopathy. Additionally, PD-like Lewy Bodies (LBs) bearing aggregated α-synuclein is present in 40-60% of all AD cases, especially involving amygdala. Amyloid deposits can be degraded or cleared by several mechanisms, including immune-mediated and transcytosis across the blood-brain barrier. Another avenue for disposal involves the lysosome pathway via autophagy. Enzymatic pathways include insulin degradative enzyme and neprilysin. Finally, the co-operative actions of C-terminus Hsp70 interacting protein (CHIP) and Parkin, components of a multiprotein E3 ubiquitin ligase complex, may be a portal to proteasome-mediated degradation. Mutations in the Parkin gene are the most common genetic link to autosomal recessive Parkinson's disease. Parkin catalyzes the post-translational modification of proteins with polyubiquitin, targeting them to the 26S proteasome. Parkin reduces intracellular Aβ(1-42) peptide levels, counteracts its effects on cell death, and reverses its effect to inhibit the proteasome. Additionally, Parkin has intrinsic cytoprotective activity to promote proteasome function and defend against oxidative stress to mitochondria. Parkin and CHIP are also active in amyloid clearance and cytoprotection in vivo. Parkin has cross-functionality in additional neurodegenerative diseases, for instance, to eliminate polyglutamine-expanded proteins, reducing their aggregation and toxicity and reinstate proteasome function. The dual actions of CHIP (molecular co-chaperone and E3 ligase) and Parkin (as E3-ubiquitin ligase and anti-oxidant) may also play a role in suppressing inflammatory reactions in animal models of neurodegeneration. In this review, we focus on the significance of CHIP and Parkin as inducers of amyloid clearance, as cytoprotectants and in the suppression of reactive inflammation. A case is made for more effort to explore whether neurodegeneration associated with proteinopathies can be arrested at early stages by promoting their mutual action.
神经退行性疾病的研究对我们理解神经生物学的更基本机制产生了重大影响。阿尔茨海默病 (AD) 和帕金森病 (PD) 的遗传学突破在轴突运输、能量代谢、蛋白质运输/清除和突触生理学等领域带来了新的知识。主要的神经退行性疾病都有一个共同的特点,即与异常蛋白质积累相关的区域性或网络病理学,以及不同程度的运动或认知能力下降。在 AD 中,β-淀粉样蛋白沉积在细胞外弥散和致密斑块以及细胞内。神经元内的 tau 病共存对疾病有很大的贡献。此外,在 40-60%的 AD 病例中,特别是涉及杏仁核的 AD 病例中,存在携带聚集的α-突触核蛋白的 PD 样路易体 (LB)。淀粉样蛋白沉积可以通过几种机制降解或清除,包括免疫介导和跨血脑屏障的转胞吞作用。另一种处理途径是通过溶酶体途径进行自噬。酶促途径包括胰岛素降解酶和 neprilysin。最后,C 端热休克蛋白 70 相互作用蛋白 (CHIP) 和 Parkin 的协同作用,Parkin 是一种多蛋白 E3 泛素连接酶复合物的组成部分,可能是蛋白酶体介导的降解的门户。Parkin 基因突变是常染色体隐性帕金森病最常见的遗传联系。Parkin 催化具有多泛素的蛋白质的翻译后修饰,将其靶向 26S 蛋白酶体。Parkin 降低细胞内 Aβ(1-42)肽水平,抵消其对细胞死亡的影响,并逆转其抑制蛋白酶体的作用。此外,Parkin 具有内在的细胞保护活性,可促进蛋白酶体功能并抵抗线粒体氧化应激。Parkin 和 CHIP 也在体内淀粉样蛋白清除和细胞保护中发挥作用。Parkin 在其他神经退行性疾病中具有交叉功能,例如消除多聚谷氨酰胺扩展蛋白,减少其聚集和毒性,并恢复蛋白酶体功能。CHIP(分子共伴侣和 E3 连接酶)和 Parkin(作为 E3-泛素连接酶和抗氧化剂)的双重作用也可能在抑制神经变性动物模型中的炎症反应中发挥作用。在这篇综述中,我们重点介绍了 CHIP 和 Parkin 作为淀粉样蛋白清除剂、细胞保护剂和抑制反应性炎症的诱导物的意义。有人提出,应该更加努力地探索是否可以通过促进它们的相互作用来阻止与蛋白病相关的神经退行性变在早期阶段进展。
