New Dipterocarpol‐Based Molecules with α‐Glucosidase Inhibitory and Hypoglycemic Activity

Author:

Smirnova Irina E.1ORCID,Galimova Zarema I.1ORCID,Sapozhnikova Tatyana A.1ORCID,Khisamutdinova Regina Yu.1ORCID,Thi Thu Ha Nguyen2ORCID,Kazakova Oxana B.1ORCID

Affiliation:

1. Ufa Institute of Chemistry, UFRC RAS 71, pr. Oktyabrya Ufa 450054 Russian Federation

2. Institute of Chemistry Vietnamese Academy of Science and Technology 18 Hoang Quoc Viet Str., Cau Giay Dist. Hanoi Vietnam

Abstract

AbstractDammarane triterpenoids are affordable and bioactive natural metabolites with great structural potential, which makes them attractive sources for drug development. The aim of the study was to investigate the potency of new dipterocarpol derivatives for the treatment of diabetes. Two dammaranes (dipterocarpol and its 20(24)‐diene derivative) were modified by a Claisen‐Schmidt aldol condensation to afford C2(E)‐arylidenes in good yields. The majority of the synthesized compounds exhibited an excellent‐to‐moderate inhibitory effect toward α‐glucosidase (from S. saccharomyces), among them eight compounds showed IC50 values less than 10 μM. 3‐Oxo‐dammarane‐2(E)‐benzylidenes (holding p‐hydroxy‐ 3 l and p‐carbonyl‐ 3 m substituents) demonstrated the most potent α‐glucosidase inhibition with IC50 0.753 and 0.204 μM, being 232‐ and 857‐times more active than acarbose (IC50 174.90 μM), and a high level of NO inhibition in Raw 264.7 cells with IC50 of 1.75 and 4.57 μM, respectively. An in vivo testing of compound 3 m (in a dose of 20 mg/kg) on a model of streptozotocin‐induced T1DM in rats showed a pronounced hypoglycemic activity, the ability to reduce effectively the processes of lipid peroxidation in liver tissue and decrease the excretion of glucose and pyruvic acid in the urine. Compound 3 m reduced the death of diabetic rats and preserved their motor activity.

Publisher

Wiley

Subject

Organic Chemistry,Molecular Biology,Molecular Medicine,Biochemistry

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