Suriya U.Duangtha C.Dontricharoen T.Yamanont P.Kuhaudomlarp S.Thitiyanuwat P.Nutho B.Arsakhant P.Saeeng R.Morales N.P.Mangmool S.Likitnukul S.Mahidol University2025-10-272025-10-272025-10-01Plos One Vol.20 No.10 October (2025)https://repository.li.mahidol.ac.th/handle/123456789/112765Type 2 diabetes mellitus (T2DM) is a global health issue associated with oxidative stress, inflammation, and insulin resistance‧ Even though α-glucosidase inhibitors such as acarbose are used in treatment, their efficacy is limited by gastrointestinal side effects‧ In this study, we evaluated the antioxidant properties and α-glucosidase inhibition of C-12 dithiocarbamate andrographolide analogues compared to the parent compound, andrographolide‧ Among all analogues, compound 3f exhibited strong antioxidant activity, achieving 84% DPPH inhibition and a reducing antioxidant power activity of 254 μM ascorbic acid equivalent (AAE) at 500 μM‧ Additionally, molecular docking suggested a favorable binding to both yeast and human α-glucosidase at a comparable level as andrographolide, verified by the surface plasmon resonance (SPR) detection system, indicating a strong binding affinity with a dissociation constant (K<inf>D</inf>) of 12‧86 μM‧ It also retains favorable physicochemical properties that align with drug-likeness based on Lipinski’s Rule‧ Functional assay confirmed its inhibitory activity with an IC<inf>50</inf> of 411 μM against the yeast α-glucosidase enzyme model, which was greater than both andrographolide and acarbose‧ Further molecular dynamics (MD) simulation analysis revealed that compound 3f exhibited stable and thermodynamically favorable binding to human α-glucosidase as well as interacting with key amino acids similar to those of andrographolide, providing a preliminary understanding of its potential relevance in a human enzyme context‧ Altogether, these findings highlight the significant potential of compound 3f as a novel α-glucosidase inhibitor, offering a potential therapeutic alternative and paving the way for further anti-diabetic drug development.MultidisciplinaryArticleSCOPUS10.1371/journal.pone.03340262-s2.0-10501921922619326203