Mechanism of Magnolia Volatile Oil in the Treatment of Acute Pancreatitis Based on GC‐MS, Network Pharmacology, and Molecular Docking

对接(动物) 机制(生物学) 化学 急性胰腺炎 药理学 医学 内科学 认识论 哲学 护理部
作者
Shengmao Li,Yu Huang,Lin Liu,Fan Zhang,Hui Ao,Yingping Luo
出处
期刊:Evidence-based Complementary and Alternative Medicine [Hindawi Publishing Corporation]
卷期号:2023 (1): 3503888-3503888 被引量:16
标识
DOI:10.1155/2023/3503888
摘要

Objective . Magnoliae officinalis cortex (MOC) is one of the most frequently used traditional Chinese medicine (TCM) for the treatment of acute pancreatitis (AP). Magnolia volatile oil (MVO) is considered to be one of the main active ingredients in MOC for AP treatment. However, the underlying mechanism of MVO in AP therapy is unknown. Methods . An integrated strategy of gas chromatography‐mass spectrum (GC‐MS), network pharmacology, and molecular docking simulation was employed to predict underlying mechanism of MVO in AP treatment. First, the compounds of MVO were identified by GC‐MS, and the targets of the identified characteristic compounds were collected from several databases, as well as AP‐related targets. Next, Gene Ontology (GO) and Kyoto Encyclopedia of Genes and Genomes (KEGG) analysis were carried out to obtain the mechanism. Moreover, the binding activity between core therapeutic targets and their corresponding compounds was evaluated by molecular docking simulation. Results . GC‐MS results showed a total of 35 compounds that appeared in at least 18 out of 20 chromatograms were considered as characteristic compounds of MVO, and 33 compounds of those were identified. Network analysis demonstrated that 33 compounds regulated 142 AP‐related targets. Of those, 8 compounds ( α ‐eudesmol, γ ‐eudesmol, (−)‐terpinen‐4‐ol, terpineol, hinesol, linalool, borneol, and β ‐eudesmol) and 8 targets (TNF, IL‐1 β , PPAR γ , PPAR α , PTGS2, NCOA1, CNR1, and ESR1) have a close relationship with AP treatment and were recognized as the key active compounds and the core therapeutic targets, respectively. The 142 targets were involved in both inflammation and calcium overload‐related biological pathways, such as neuroactive ligand‐receptor interaction, estrogen, MAPK, and calcium signaling pathway. Moreover, molecular docking simulation indicated that the 8 core therapeutic targets strongly interacted with their corresponding compounds. Conclusions . In summary, the present study elucidated that the efficacy of MVO in AP treatment might be attributed to anti‐inflammation and inhibition of calcium overload through multicomponents and multitargets.
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