| Title : Highly potent dipeptidyl peptidase IV inhibitors derived from Alogliptin through pharmacophore hybridization and lead optimization - Xie_2013_Eur.J.Med.Chem_68_312 |
| Author(s) : Xie H , Zeng L , Zeng S , Lu X , Zhao X , Zhang G , Tu Z , Xu H , Yang L , Zhang X , Wang S , Hu W |
| Ref : Eur Journal of Medicinal Chemistry , 68 :312 , 2013 |
|
Abstract :
The superposition of the DPP-IV complex revealed that the butynyl group of Linagliptin can be freely switched with the cyanobenzyl group of Alogliptin. Thus, a pharmacophore hybridization of Alogliptin was initiated and led to a novel DPP-IV inhibitor, 11a. Although it did not exhibit the desired activity (IC50=0.2 microM), compound 11a acts as a lead compound, which triggered a resulting structural optimization and the formation of compound 11m. A novel series of potent DPP-IV inhibitors represented by compound 11m (IC50=0.4 nM) was ultimately obtained with a robust pharmacokinetic profile and superior in vitro and in vivo efficacy compared to Alogliptin. |
| PubMedSearch : Xie_2013_Eur.J.Med.Chem_68_312 |
| PubMedID: 23994324 |
Xie H, Zeng L, Zeng S, Lu X, Zhao X, Zhang G, Tu Z, Xu H, Yang L, Zhang X, Wang S, Hu W (2013)
Highly potent dipeptidyl peptidase IV inhibitors derived from Alogliptin through pharmacophore hybridization and lead optimization
Eur Journal of Medicinal Chemistry
68 :312
Xie H, Zeng L, Zeng S, Lu X, Zhao X, Zhang G, Tu Z, Xu H, Yang L, Zhang X, Wang S, Hu W (2013)
Eur Journal of Medicinal Chemistry
68 :312