What question did this study set out to answer?

The aim is to assess the synthesis and multifunctional bioactivities of oxadiazolo-benzodiazepines.

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March 1, 2026

Bioactive oxadiazolo-benzodiazepines: synthesis, α amylase inhibition, antioxidant activity, molecular docking and DFT calculation.

Key Points

The aim is to assess the synthesis and multifunctional bioactivities of oxadiazolo-benzodiazepines.
Synthesis of diastereoisomers 3 and 4 of oxadiazolo-benzodiazepines.
Evaluation of alpha-amylase inhibition using IC50 values.
Assessment of antioxidant activity through DPPH scavenging.
Molecular docking studies to analyze binding interactions.
DFT calculations to study molecular properties.
Compound 3 demonstrated strong alpha-amylase inhibition with IC50 of 22.78 µM.
Compound 4 showed significant antioxidant activity with IC50 of 68.16 μM.
Both compounds outperformed standard drugs like Acarbose and ascorbic acid.
Molecular docking confirmed effective binding to enzyme active sites.

Abstract

Both diastereoisomers 3 and 4 demonstrated superior activity compared to standard drugs. Compound 3 showed potent α-amylase inhibition IC50 = 22.78 µM) compared to Acarbose IC50 = 123 µM). For antioxidant activity, compounds 4 and 3 exhibited strong DPPH scavenging IC50 = 68.16 and 79.50 μM, respectively), outperforming ascorbic acid. Docking studies confirmed favorable binding interactions within the active sites of target enzymes. The synthesized oxadiazolo-benzodiazepines represent promising multifunctional antidiabetic and antioxidant candidates, warranting further pharmacological investigation.

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Bioactive oxadiazolo-benzodiazepines: synthesis, α amylase inhibition, antioxidant activity, molecular docking and DFT calculation.

Key Points

Abstract

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