Department of Chemistry, Université de Montréal, Station Centre-Ville, C.P. 6128, Montreal, QC H3C 3J7, Canada.
Institut de Recherches Servier, 125 Chemin de Ronde, 78290 Croissy, France.
Bioorg Med Chem Lett. 2022 Nov 1;75:128950. doi: 10.1016/j.bmcl.2022.128950. Epub 2022 Aug 24.
We describe the synthesis of a series of 3-t-butyl 5-aminopyrazole p-substituted arylamides as inhibitors of serine-threonine25 (STK25), an enzyme implicated in the progression of non-alcoholic fatty liver disease (NAFLD). Appending a p-N-pyrrolidinosulphonamide group to the arylamide group led to a 'first-in kind' inhibitor with IC = 228 nM. A co-crystal structure with STK 25 revealed productive interactions which were also reproduced using molecular docking. A new series of triazolo dihydro oxazine carboxamides of 3-t-butyl 5-aminopyrazole was not active against STK25.
我们描述了一系列 3-叔丁基 5-氨基吡唑对取代芳酰胺的合成,这些化合物是丝氨酸-苏氨酸 25(STK25)的抑制剂,STK25 酶与非酒精性脂肪性肝病(NAFLD)的进展有关。在芳酰胺基团上附加一个对- N-吡咯烷磺酰胺基团,得到了一种“首例”的抑制剂,IC = 228 nM。与 STK 25 的共晶结构揭示了具有生产性相互作用,这些相互作用也可以通过分子对接来重现。一系列新的 3-叔丁基 5-氨基吡唑三唑并二氢恶嗪甲酰胺对 STK25 没有活性。
