Targeting Hypoglycemic Natural Products from the Cloud Forest Plants Using Chemotaxonomic Computer-Assisted Selection

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Dades bibliogràfiques
Publicat a:	International Journal of Molecular Sciences vol. 25, no. 20 (2024), p. 10881
Autor principal:	Mayo-Montor, Cecilia I
Altres autors:	Vidal-Limon, Abraham, Loyola-Vargas, Víctor Manuel, Carmona-Hernández, Oscar, José Martín Barreda-Castillo, Monribot-Villanueva, Juan L, Guerrero-Analco, José A
Publicat:	MDPI AG
Matèries:	Mexico Glucagon Hyperglycemia Metabolism Flowers & plants Libraries Natural products Enzymes Metabolites Carbohydrates
Accés en línia:	Citation/Abstract Full Text + Graphics Full Text - PDF
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Descripció
Resum:	The cloud forest (CF), a hugely biodiverse ecosystem, is a hotspot of unexplored plants with potential for discovering pharmacologically active compounds. Without sufficient ethnopharmacological information, developing strategies for rationally selecting plants for experimental studies is crucial. With this goal, a CF metabolites library was created, and a ligand-based virtual screening was conducted to identify molecules with potential hypoglycemic activity. From the most promising botanical families, plants were collected, methanolic extracts were prepared, and hypoglycemic activity was evaluated through in vitro enzyme inhibition assays on α-amylase, α-glucosidase, and dipeptidyl peptidase IV (DPP-IV). Metabolomic analyses were performed to identify the dominant metabolites in the species with the best inhibitory activity profile, and their affinity for the molecular targets was evaluated using ensemble molecular docking. This strategy led to the identification of twelve plants (in four botanical families) with hypoglycemic activity. Sida rhombifolia (Malvaceae) stood out for its DPP-IV selective inhibition versus S. glabra. A comparison of chemical profiles led to the annotation of twenty-seven metabolites over-accumulated in S. rhombifolia compared to S. glabra, among which acanthoside D and cis-tiliroside were noteworthy for their potential selective inhibition due to their specific intermolecular interactions with relevant amino acids of DPP-IV. The workflow used in this study presents a novel targeting strategy for identifying novel bioactive natural sources, which can complement the conventional selection criteria used in Natural Product Chemistry.
ISSN:	1661-6596 1422-0067
DOI:	10.3390/ijms252010881
Font:	Health & Medical Collection