Lau Lit-Fui, Seymour Patricia A, Sanner Mark A, Schachter Joel B
CNS Discovery, Pfizer Global Research and Development, Groton, CT 06340, USA.
J Mol Neurosci. 2002 Dec;19(3):267-73. doi: 10.1385/JMN:19:3:267.
Cyclin-dependent kinase-5 (cdk5) is suggested to play a role in tau phosphorylation and contribute to the pathogenesis of Alzheimer's disease (AD). One of its activators, p25, is dramatically increased in AD brains where p25 and cdk5 are colocalized with neurofibrillary tangles. Several animal models have shown a correlation of p25/cdk5 activities with tau phosphorylation. Overexpression of p25/cdk5 in nueronal cultures not only leads to tau phosphorylation but also cytoskeletal abnormalities and neurodegeneration. Therefore, cdk5 kinase inhibitors are potential therapeutic agents for the treatment of AD. Availability of potent, selective, brain permeable cdk5 inhibitors and relevant animal models in which their efficacy can be treated will be critical in the development of these inhibitors.
细胞周期蛋白依赖性激酶5(cdk5)被认为在tau蛋白磷酸化过程中发挥作用,并促使阿尔茨海默病(AD)的发病。其激活剂之一p25在AD脑内显著增加,且p25和cdk5与神经原纤维缠结共定位。多个动物模型已显示p25/cdk5活性与tau蛋白磷酸化之间存在关联。在神经元培养物中过表达p25/cdk5不仅会导致tau蛋白磷酸化,还会引起细胞骨架异常和神经退行性变。因此,cdk5激酶抑制剂是治疗AD的潜在治疗药物。高效、选择性、可透过血脑屏障的cdk5抑制剂以及能够评估其疗效的相关动物模型的可得性,对于这些抑制剂的研发至关重要。
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