Institute for Neurodegenerative Diseases, San Francisco, CA 94143-0518, USA.
J Virol. 2010 Apr;84(7):3408-12. doi: 10.1128/JVI.02145-09. Epub 2009 Dec 23.
Prion diseases are fatal, untreatable neurodegenerative diseases caused by the accumulation of the misfolded, infectious isoform of the prion protein (PrP), termed PrP(Sc). In an effort to identify novel inhibitors of prion formation, we utilized a high-throughput enzyme-linked immunosorbent assay (ELISA) to evaluate PrP(Sc) reduction in prion-infected neuroblastoma cell lines (ScN2a). We screened a library of approximately 10,000 diverse small molecules in 96-well format and identified 121 compounds that reduced PrP(Sc) levels at a concentration of 5 microM. Four chemical scaffolds were identified as potential candidates for chemical optimization based on the presence of preliminary structure-activity relationships (SAR) derived from the primary screening data. A follow-up analysis of a group of commercially available 2-aminothiazoles showed this class as generally active in ScN2a cells. Our results establish 2-aminothiazoles as promising candidates for efficacy studies of animals and validate our drug discovery platform as a viable strategy for the identification of novel lead compounds with antiprion properties.
朊病毒病是由朊病毒蛋白(PrP)的错误折叠、传染性异构体(称为 PrP(Sc))积累引起的致命、不可治疗的神经退行性疾病。为了鉴定新型朊病毒形成抑制剂,我们利用高通量酶联免疫吸附测定(ELISA)评估了朊病毒感染的神经母细胞瘤细胞系(ScN2a)中 PrP(Sc)的减少。我们以 96 孔格式筛选了约 10000 种不同的小分子文库,并鉴定出 121 种在 5μM 浓度下降低 PrP(Sc)水平的化合物。基于初步的构效关系(SAR)从初级筛选数据中得出,根据存在的 4 种化学结构支架被确定为化学优化的潜在候选物。对一组市售的 2-氨基噻唑的后续分析表明,该类化合物在 ScN2a 细胞中普遍具有活性。我们的结果将 2-氨基噻唑确立为动物疗效研究的有希望的候选物,并验证了我们的药物发现平台作为鉴定具有抗朊病毒特性的新型先导化合物的可行策略。
