Tas_2025_Future.Med.Chem__1

Reference

Title : Pyrrolidine-based hybrid compounds: design, synthesis, in vitro and in vivo pharmacological properties and molecular docking studies - Tas_2025_Future.Med.Chem__1
Author(s) : Tas S , Dondas HA , Yaktubay Dondas N , Poyraz S , Tok TT , Demiray GA , Belveren S , Ince T , Demir Y , Yilmaz MB , Ulger M , Tamer MA , Sansano JM , Pask CM
Ref : Future Med Chem , :1 , 2025
Abstract :

AIMS: To design, synthesize, and evaluate pyrrolidine-based hybrids bearing indole, thiourea, and vinyl sulfone pharmacophores as dual inhibitors of human carbonic anhydrase I/II (hCAI/II) and acetylcholinesterase (AChE), with secondary profiling of complementary bioactivities. MATERIALS & METHODS: Three hybrids (6a, 6b, 8) were obtained via imine azomethine ylide 1,3-dipolar cycloaddition and derivatization. Structures were confirmed spectroscopically and assayed in vitro for hCAI/II and AChE inhibition. Additional evaluations included antioxidant (DPPH), antibacterial, antifungal, antituberculosis (M. tuberculosis H37Rv), cytotoxicity (HCT116, DPSCs), anti-inflammatory (COX-2, SOD1 ELISA, mouse xylene-induced), antidepressant (forced swim test), molecular docking, and in silico ADMET. RESULTS: Compound 6b was the most potent inhibitor (hCAII Ki 75.79 +/- 2.83 nM, AChE Ki 43.17 +/- 10.44 nM), outperforming acetazolamide (Ki 299.33 +/- 45.44 nM) and tacrine (Ki 103.47 +/- 11.54 nM). Compound 6a showed the strongest antioxidant effect (72.30% DPPH), antibacterial activity against A. baumannii (MIC 125 microg/ml, comparable to ampicillin), and superior anti-TB potency (MIC 31.25 microg/ml). Compound 6b exhibited stronger antibacterial activity (MIC 62.5 microg/ml). Both reduced COX-2 levels, and 6a increased SOD1. The hybrids were selectively cytotoxic to HCT116, sparing DPSCs. Docking studies confirmed key binding interactions, while ADMET predicted favorable profiles. . CONCLUSIONS: The hybrids validate a focused dual-target strategy. Compound 6b is the most potent hCAII and AChE inhibitor, while 6a emerges as a broader multi-target lead with antioxidant, antimicrobial, anti-inflammatory, and antidepressant potential.

PubMedSearch : Tas_2025_Future.Med.Chem__1
PubMedID: 40955181

Related information

Citations formats

Tas S, Dondas HA, Yaktubay Dondas N, Poyraz S, Tok TT, Demiray GA, Belveren S, Ince T, Demir Y, Yilmaz MB, Ulger M, Tamer MA, Sansano JM, Pask CM (2025)
Pyrrolidine-based hybrid compounds: design, synthesis, in vitro and in vivo pharmacological properties and molecular docking studies
Future Med Chem :1

Tas S, Dondas HA, Yaktubay Dondas N, Poyraz S, Tok TT, Demiray GA, Belveren S, Ince T, Demir Y, Yilmaz MB, Ulger M, Tamer MA, Sansano JM, Pask CM (2025)
Future Med Chem :1