Exploring the inhibitory properties of biflavonoids on α-glucosidase; computational and experimental approaches

Morteza Sadeghi; Mehran Miroliaei; Mustafa Ghanadian; Antoni Szumny; Mehdi Rahimmalek

doi:10.1016/j.ijbiomac.2023.127380

Exploring the inhibitory properties of biflavonoids on α-glucosidase; computational and experimental approaches

Int J Biol Macromol. 2023 Dec 31;253(Pt 7):127380. doi: 10.1016/j.ijbiomac.2023.127380. Epub 2023 Oct 12.

Authors

Morteza Sadeghi¹, Mehran Miroliaei², Mustafa Ghanadian³, Antoni Szumny⁴, Mehdi Rahimmalek⁵

Affiliations

¹ Faculty of Biological Science and Technology, Department of Cell and Molecular Biology & Microbiology, University of Isfahan, Isfahan, Iran. Electronic address: mo.sadeghi@sci.ui.ac.ir.
² Faculty of Biological Science and Technology, Department of Cell and Molecular Biology & Microbiology, University of Isfahan, Isfahan, Iran. Electronic address: m.miroliaei@sci.ui.ac.ir.
³ Department of Pharmacognosy, Isfahan University of Medical Sciences, Isfahan, Iran.
⁴ Department of Food Chemistry and Biocatalysis, Wrocław University of Environmental and Life Sciences, 50-375 Wrocław, Poland.
⁵ Department of Food Chemistry and Biocatalysis, Wrocław University of Environmental and Life Sciences, 50-375 Wrocław, Poland; Department of Horticulture, College of Agriculture, Isfahan University of Technology, 84156-83111 Isfahan, Iran.

PMID: 37838108
DOI: 10.1016/j.ijbiomac.2023.127380

Abstract

Biflavonoids (BFs) are a group of polyphenols that have a unique biochemical structure. One of the key biomedical mechanisms that BFs can have high potential in managing Diabetes mellitus (DM) is α-glucosidase inhibition. Normally, elevated blood glucose levels are caused by high absorption of glucose in the epithelium of the small intestine. Since α-glucosidase helps increase the absorption of glucose in the small intestine in the final stage of glycan catabolism, inhibition of this essential biochemical process in diabetic patients can be considered a suitable approach in the treatment of this disease. The interaction between the BFs and α-glucosidase are still not clear, and need to be deeply investigated. Herein, the aim is to identify BFs with strong α-glucosidase inhibitory activity. Using docking-based virtual screening approach, the potential binding affinity of 18 selected BFs to α-glucosidase was evaluated. The dynamic activity and stability of α-glucosidase-BFs complexes were then measured by molecular dynamics simulation (MDs). "Strychnobiflavone" showed the best score in α-glucosidase inhibition. Arg315 and Phe303 involved in the interactions of α-glucosidase-strychnobiflavone complex through cation-π and π-π stacking, respectively. Based on in vitro kinetic studies, it was determined that the type of inhibition of "strychnobiflavone" corresponds to the pattern of mixed inhibitors. Furthermore, details of the interactions between strychnobiflavone and α-glucosidase were performed by in silico secondary structure content analysis. The findings showed when "strychnobifone" binds to the enzyme, significant alterations occur in the enzyme conformation affecting its catalytic activity. In general, the findings highlighted the potential of "strychnobiflavone" as a promising candidate for the treatment of diabetes mellitus through α-glucosidase inhibition. Further in vitro and in vivo studies have to confirm the therapeutic benefits of "strychnobiflavone" in conformational diseases such as diabetes mellitus.

Keywords: Biflavonoids; Diabetes mellitus; Mix-inhibition; Strychnobiflavone; α-Glucosidase.

MeSH terms

Biflavonoids* / pharmacology
Diabetes Mellitus*
Glucose
Glycoside Hydrolase Inhibitors / chemistry
Humans
Kinetics
Molecular Docking Simulation
alpha-Glucosidases / metabolism

Substances

alpha-Glucosidases
Glycoside Hydrolase Inhibitors
Biflavonoids
Glucose