Fiolek Taylor J, Magyar Christina L, Wall Tyler J, Davies Steven B, Campbell Molly V, Savich Christopher J, Tepe Jetze J, Mosey R Adam
Department of Chemistry, Michigan State University, East Lansing, MI 48824, United States.
Department of Chemistry, Lake Superior State University, Sault Sainte Marie, MI 49783, United States.
Bioorg Med Chem Lett. 2021 Mar 15;36:127821. doi: 10.1016/j.bmcl.2021.127821. Epub 2021 Jan 27.
Aggregates or oligomeric forms of many intrinsically disordered proteins (IDPs), including α-synuclein, are hallmarks of neurodegenerative diseases, like Parkinson's and Alzheimer's disease, and key contributors to their pathogenesis. Due to their disordered nature and therefore lack of defined drug-binding pockets, IDPs are difficult targets for traditional small molecule drug design and are often referred to as "undruggable". The 20S proteasome is the main protease that targets IDPs for degradation and therefore small molecule 20S proteasome enhancement presents a novel therapeutic strategy by which these undruggable IDPs could be targeted. The concept of 20S activation is still relatively new, with few potent activators having been identified thus far. Herein, we synthesized and evaluated a library of dihydroquinazoline analogues and discovered several promising new 20S proteasome activators. Further testing of top hits revealed that they can enhance 20S mediated degradation of α-synuclein, the IDP associated with Parkinson's disease.
许多内在无序蛋白质(IDP)的聚集体或寡聚形式,包括α-突触核蛋白,是神经退行性疾病(如帕金森病和阿尔茨海默病)的标志,也是其发病机制的关键因素。由于其无序的性质,因此缺乏明确的药物结合口袋,IDP是传统小分子药物设计的困难靶点,通常被称为“不可成药”。20S蛋白酶体是将IDP靶向降解的主要蛋白酶,因此小分子增强20S蛋白酶体提供了一种新的治疗策略,通过该策略可以靶向这些不可成药的IDP。20S激活的概念仍然相对较新,到目前为止仅鉴定出少数强效激活剂。在此,我们合成并评估了二氢喹唑啉类似物库,并发现了几种有前景的新型20S蛋白酶体激活剂。对顶级命中物的进一步测试表明,它们可以增强20S介导的与帕金森病相关的IDPα-突触核蛋白的降解。
