Exploring the underlying mechanisms of fisetin in the treatment of hepatic insulin resistance via network pharmacology and in vitro validation

Tian Li; Junjun Ling; Xingrong Du; Siyu Zhang; Yan Yang; Liang Zhang

doi:10.1186/s12986-023-00770-z

Nutrition & Metabolism (Nov 2023)

Exploring the underlying mechanisms of fisetin in the treatment of hepatic insulin resistance via network pharmacology and in vitro validation

Tian Li,
Junjun Ling,
Xingrong Du,
Siyu Zhang,
Yan Yang,
Liang Zhang

Affiliations

Tian Li: Metabilic Vascular Disease Key Laboratory of Sichuan Province
Junjun Ling: Affiliated Hospital of Guizhou Medical University
Xingrong Du: Metabilic Vascular Disease Key Laboratory of Sichuan Province
Siyu Zhang: Drug Discovery Research Center, Southwest Medical University
Yan Yang: Chongqing Tongnan NO.1 Middle School
Liang Zhang: Metabilic Vascular Disease Key Laboratory of Sichuan Province

DOI: https://doi.org/10.1186/s12986-023-00770-z
Journal volume & issue: Vol. 20, no. 1
pp. 1 – 14

Abstract

Read online

Abstract Objective To characterize potential mechanisms of fisetin on hepatic insulin resistance (IR) using network pharmacology and in vitro validation. Methods Putative targets of fisetin were retrieved from the Traditional Chinese Medicine Systems Pharmacology database, whereas the potential genes of hepatic IR were obtained from GeneCards database. A protein–protein interaction (PPI) network was constructed according to the intersection targets of fisetin and hepatic IR using the Venn diagram. The biological functions and potential pathways related to genes were determined using Gene Ontology (GO) and Kyoto Encyclopedia of Genes and Genomes (KEGG) analyses. Cell experiments were also conducted to further verify the mechanism of fisetin on hepatic IR. Results A total of 118 potential targets from fisetin were associated with hepatic IR. The areas of nodes and corresponding degree values of TP53, AKT1, TNF, IL6, CASP3, CTNNB1, JUN, SRC, epidermal growth factor receptor (EGFR), and HSP90AA1 were larger and could be easily found in the PPI network. Furthermore, GO analysis revealed that these key targets were significantly involved in multiple biological processes that participated in oxidative stress and serine/threonine kinase activity. KEGG enrichment analysis showed that the PI3K/AKT signaling pathway was a significant pathway involved in hepatic IR. Our in vitro results demonstrated that fisetin treatment increased the expressions of EGFR and IRS in HepG2 and L02 cells under normal or IR conditions. Western blot results revealed that p-AKT/AKT levels were significantly up-regulated, suggesting that fisetin was involved in the PI3K/AKT signaling pathway to regulate insulin signaling. Conclusion We explored the pharmacological actions and the potential molecular mechanism of fisetin in treating hepatic IR from a holistic perspective. Our study lays a theoretical foundation for the development of fisetin for type 2 diabetes.

Published in Nutrition & Metabolism

ISSN: 1743-7075 (Online)
Publisher: BMC
Country of publisher: United Kingdom
LCC subjects: Technology: Home economics: Nutrition. Foods and food supply; Medicine: Internal medicine: Specialties of internal medicine: Nutritional diseases. Deficiency diseases
Website: https://nutritionandmetabolism.biomedcentral.com/

About the journal

Abstract

Keywords