Youdim M B H, Fridkin M, Zheng H
Eve Topf and National Parkinson Foundation Centers of Excellence for Neurodegenerative Diseases Research, and Department of Pharmacology, Technion-Rapapport Faculty of Medicine, Haifa, Israel.
J Neural Transm (Vienna). 2004 Oct;111(10-11):1455-71. doi: 10.1007/s00702-004-0143-x. Epub 2004 Apr 20.
Iron has been shown to accumulates at site where neurons degenerate in neurodegenerative diseases of Parkinson's disease, Alzheimer's disease, Huntington disease, amyotrophic lateral sclerosis and Friedreich ataxia. Iron is thought to participate or initiate oxidative stress via generation of reactive oxygen species (ROS), such as hydroxyl radical. Iron chelators are neuroprotective and prevent 6-hydroxydoapmine and MPTP dopaminergic neurotoxicity in rats and mice. However, their action on monoamine oxidase (MAO) A and B have not been determined previously since MAO-B inhibitors have been shown to be neuroprotective in cellular and animal models of Parkinson's disease. The chelators 8-hydroxyquinoline, O-phenanthroline, 2,2'-dipyridyl, U74500A and U74600F showed a preference for inhibition of rat brain mitochondrial MAO-A over MAO-B. Their IC(50) ranged from 10(-3) M to 10(-6) M, with 21-amino steroids (U74500A and U74006F) showing a greater selectivity and potency for MAO-A. Desferrioxamine (desferal), a prototype potent iron chelator, exhibited relatively poor MAO inhibitory. The inhibitions of MAO-A and B by 21-amino steroids (Lazaroids) were time dependent and irreversible. Those initiated by 8-hydroxyquinoline, 2,2'-dipyridyl and O-phenanthroline were fully reversible by enzyme dilution experiments. Both Fe(2+) and Fe(3+) reverse the MAO-A and B inhibition induced by the latter chelators, but not those initiated by 21-amino steroids. The data infer that either the inhibition of MAO by 21-amino steroids is either the resultant of their conversion to an irreversible covalently bound ligand or that the iron chelation moiety and MAO inhibitory activity in these compounds are not mutually shared. The results suggest that bifunctional brain penetrable drugs with iron chelating property and MAO inhibitory activity in could be the most feasible approach for neuroprotection in neurodegenerative diseases. Such drug would prevent participation of elevated iron in oxidative stress and formation of reactive hydroxyl radical, via its interaction with H(2)O2 (Fenton chemistry), generated as a consequence MAO and other oxidative enzyme reactions to generative cytotoxic reactive hydroxyl radical. We have now developed several of these compounds with neuroprotective, MAO inhibitory and iron chelating properties from our prototype iron chelators, VK-28 possessing propargylamine moiety of our anti-parkinson drug, rasagiline.
铁已被证明会在帕金森病、阿尔茨海默病、亨廷顿病、肌萎缩侧索硬化症和弗里德赖希共济失调等神经退行性疾病中神经元退化的部位蓄积。铁被认为通过产生活性氧(ROS),如羟基自由基,参与或引发氧化应激。铁螯合剂具有神经保护作用,可预防大鼠和小鼠体内6-羟基多巴胺和MPTP诱导的多巴胺能神经毒性。然而,由于已证明单胺氧化酶(MAO)-B抑制剂在帕金森病的细胞和动物模型中具有神经保护作用,所以此前尚未确定铁螯合剂对MAO-A和B的作用。螯合剂8-羟基喹啉、邻菲罗啉、2,2'-联吡啶、U74500A和U74600F对大鼠脑线粒体MAO-A的抑制作用优于MAO-B。它们的半数抑制浓度(IC50)范围为10-3 M至10-6 M,其中21-氨基类固醇(U74500A和U74006F)对MAO-A表现出更高的选择性和效力。去铁胺(去铁酮)作为一种典型的强效铁螯合剂,对MAO的抑制作用相对较弱。21-氨基类固醇(拉扎罗类化合物)对MAO-A和B的抑制作用具有时间依赖性且不可逆。由8-羟基喹啉、2,2'-联吡啶和邻菲罗啉引发的抑制作用可通过酶稀释实验完全逆转。Fe2+和Fe3+均可逆转后一种螯合剂诱导的MAO-A和B的抑制作用,但不能逆转21-氨基类固醇引发的抑制作用。这些数据表明,要么21-氨基类固醇对MAO的抑制作用是其转化为不可逆共价结合配体的结果,要么这些化合物中的铁螯合部分和MAO抑制活性并非相互共享。结果表明,具有铁螯合特性和MAO抑制活性的双功能可穿透脑的药物可能是神经退行性疾病神经保护最可行的方法。这类药物可通过与MAO和其他氧化酶反应产生的细胞毒性活性羟基自由基所生成的H2O2(芬顿化学)相互作用,防止升高的铁参与氧化应激和活性羟基自由基的形成。我们现已从我们的原型铁螯合剂VK-28开发出几种具有神经保护、MAO抑制和铁螯合特性的化合物,VK-28含有我们的抗帕金森药物雷沙吉兰的炔丙胺部分。
