What question did this study set out to answer?

The aim is to develop novel dual inhibitors targeting α-glucosidase and PTP1B for treating diabetes.

May 8, 2026Open Access

Design, synthesis and biological evaluation of novel coumarin-1, 2, 4-triazole derivatives as dual inhibitors of α-glucosidase and PTP1B

Key Points

The aim is to develop novel dual inhibitors targeting α-glucosidase and PTP1B for treating diabetes.
Fourteen coumarin-1, 2, 4-triazole derivatives were synthesized and evaluated for their inhibitory activity in vitro.
Compound 10n was further analyzed for binding interactions using molecular docking.
In vivo experiments were conducted in Kunming mice to assess postprandial blood sugar levels.
Compound 10n exhibited significant α-glucosidase inhibition with an IC50 of 9.71 ± 0.28 μM, compared to acarbose (IC50: 309.83 ± 8.74 μM).
10n also showed PTP1B inhibitory activity with an IC50 of 7.31 ± 1.55 μM, better than ursolic acid (IC50: 4.55 ± 1.08 μM).
In vivo, 10n at 20 mg/kg reduced postprandial blood sugar levels in mice significantly.

Abstract

Multi-target inhibitors are one of the important directions in the current research on anti-diabetic drugs. To develop new dual-target inhibitors of protein tyrosine phosphatase 1B (PTP1B) and α-glucosidase, fourteen coumarin-1, 2, 4-triazole derivatives ( 10a-10n ) were design and synthesized. All synthetic compounds were screened for their in vitro α-glucosidase inhibitory activity by using yeast α-glucosidase enzyme. In comparison with the positive acarbose (IC 50 : 309.83 ± 8.74 μM), these derivatives had moderate to high active inhibitory activity against α-glucosidase with IC 50 values between 9.71 ± 0.28 μM and 160.67 ± 5.10 μM. In addition, the most active compound 10n also exhibits PTP1B inhibitory activity as compared to the positive ursolic acid (IC 50: 4.55 ± 1.08 μM), with an IC 50 value of 7.31 ± 1.55 μM. SAR analysis demonstrated a significant improvement in α-glucosidase inhibitory activity upon the introduction of substituents with increased steric hindrance. α-Glucosidase inhibition mechanism experiments demonstrate that 10n is a mixed-type inhibitor. Compound 10n reduced the fluorescence intensity of glucosidase by 47.5% through a static quenching manner. The outcome of synchronous fluorescence indicated the location where 10n bound to the protein was closer to tryptophan residue. The results of CD (α-helix: 36.8% to 26.9%; β-sheets: 15.5% to 21.4%; β-turns: 16.3% to 18.1%; random coils: 29.4% to 37.3%) and 3D fluorescence (reduce the fluorescence intensity of characteristic peak 1 and 2) demonstrated the addition of compound 10n could destroy the original conformation of α-glucosidase. Importantly, molecular docking uncovered 10n could enter active pockets both α-glucosidase (binding energy: -11.7 kcal•mol -1 ) and PTP1B (binding energy: -8.3 kcal•mol -1 ) and interacted with residues through hydrogen bond, hydrophobic contact, π-π stacking interaction. The in vivo experiment found 10n (20 mg/kg, n = 8) could lower postprandial blood sugar levels in Kunming mice (ethical approval has been obtained).

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Design, synthesis and biological evaluation of novel coumarin-1, 2, 4-triazole derivatives as dual inhibitors of α-glucosidase and PTP1B

Key Points

Abstract

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