Decoding the mechanism of Eleutheroside E in treating osteoporosis via network pharmacological analysis and molecular docking of osteoclast-related genes and gut microbiota

Tianyu Zhou; Yilin Zhou; Dongdong Ge; Youhong Xie; Jiangyan Wang; Lin Tang; Qunwei Dong; Ping Sun

doi:10.3389/fendo.2023.1257298

Decoding the mechanism of Eleutheroside E in treating osteoporosis via network pharmacological analysis and molecular docking of osteoclast-related genes and gut microbiota

Front Endocrinol (Lausanne). 2023 Nov 7:14:1257298. doi: 10.3389/fendo.2023.1257298. eCollection 2023.

Authors

Tianyu Zhou^#¹, Yilin Zhou^#¹, Dongdong Ge², Youhong Xie¹, Jiangyan Wang¹, Lin Tang¹, Qunwei Dong^{2

3}, Ping Sun¹

Affiliations

¹ Department of Endocrinology, The First Affiliated Hospital of Guangdong Pharmaceutical University, Guangzhou, China.
² Department of Orthopedics, The First Affiliated Hospital of Guangdong Pharmaceutical University, Guangzhou, China.
³ Department of Orthopedics, Yunfu Hospital of Traditional Chinese Medicine, Yunfu, China.

^# Contributed equally.

Abstract

Objective: Eleutheroside E (EE) is an anti-inflammatory natural compound derived from the edible medicinal herb Acanthopanax senticosus. This study aims to investigate the underlying mechanism of the anti-osteoporosis action of EE through network pharmacology, molecular docking and gut microbiota.

Materials and methods: Network pharmacology was used to explore the potential core targets and main pathways mediated by EE in osteoporosis (OP) treatment. Molecular docking was exploited to investigate the interactions between the active anti-OP compounds in EE and the potential downstream targets. Following the multi-approach bioinformatics analysis, ovariectomy (OVX) model was also established to investigate the in vivo anti-OP effects of EE.

Results: The top 10 core targets in PPI network were TP53, AKT1, JUN, CTNNB1, STAT3, HIF1A, EP300, CREB1, IL1B and ESR1. Molecular docking results that the binding energy of target proteins and the active compounds was approximately between -5.0 and -7.0 kcal/mol, which EE has the lowest docking binding energy with HIF1A. Enrichment analysis of GO and KEGG pathways of target proteins indicated that EE treatment could potentially alter numerous biological processes and cellular pathways. In vivo experiments demonstrated the protective effect of EE treatment against accelerated bone loss, where reduced serum levels of TRAP, CTX, TNF-α, LPS, and IL-6 and increased bone volume and serum levels of P1NP were observed in EE-treated mice. In addition, changes in gut microbiota were spotted by 16S rRNA gene sequencing, showing that EE treatment increased the relative abundance of Lactobacillus and decreased the relative abundance of Clostridiaceae.

Conclusion: In summary, these findings suggested that the characteristics of multi-target and multi-pathway of EE against OP. In vivo, EE prevents the onset of OP by regulating gut microbiota and inflammatory response and is therefore a potential OP drug.

Keywords: Eleutheroside E (EE); gut microbiota; molecular docking; network pharmacology; postmenopausal osteoporosis (PMO).

Publication types

Research Support, Non-U.S. Gov't

MeSH terms

Animals
Female
Gastrointestinal Microbiome*
Mice
Molecular Docking Simulation
Osteoclasts
Osteoporosis* / drug therapy
Osteoporosis* / genetics
RNA, Ribosomal, 16S

Substances

eleutheroside E
RNA, Ribosomal, 16S

Grants and funding

The author(s) declare financial support was received for the research, authorship, and/or publication of this article. This work was supported by grants from the National Science Foundation for Young Scholars, China [No. 81603641], Science and Technology Planning Project of Yunfu, Guangdong Province, China [No. 2020A090402].