Exploring the Pharmacological Action Mechanism of Chamomile Essential Oil on the Treatment of Breast Cancer Based on Network Pharmacology

Author:

Maitisha Guzhalinuer1,Zhou Junhao2,Zhao Youyun1,Liu Guangzhong1,Zhao Yan1,Zheng Yi1,Li Ling1,Han Shuxia1,Peng Li1,Abliz Ablikim1

Affiliation:

1. Hubei Provincial Hospital of Traditional Chinese Medicine, Hubei Province Academy of Traditional Chinese Medicine

2. Hubei University of Chinese Medicine

Abstract

Abstract Background Chamomile essential oil (CEO) can be beneficial in cancer therapy. The aim of the current research is to explore the underlying mechanism of CEO for breast cancer treatment by network pharmacology approach and evaluate its anti-breast cancer capacity in vitro. Methods We extracted CEO from chamomile flowers and analyzed its chemical components by using GC-MS/MS. Network pharmacology method was employed to screen the active components, potential targets and possible mechanism of CEO for breast cancer treatment. The molecular docking was used to validated the results of network pharmacology. Cell viability, apoptosis and cell cycle assay were used to assess anti-breast cancer effect of CEO. Results In network pharmacology analysis, we found the 12 effective components and 265 drug-disease common targets of CEO and among them, five active components and 19 targets were determined as the therapeutic targets of breast cancer. GO results demonstrated that the potenributetial targets of CEO were primarily participated in positive regulation of MAPK cascade, distd in membrane raft and the molecular functions were associated with protein serine-threonine-tyrosine kinase activity. KEGG pathway analysis suggested that the potential targets mainly involved in PI3K-AKT signaling pathway, cAMP signaling pathway, neuroactive ligand-receptor interaction, MAPK signaling pathway and calcium signaling pathway. Molecular docking analysis revealed that LYN, LCK, VGFR, MAPK11, MAPK14, PTK2, JAK1, NR3C1 and ESR1 have shown higher affinity with three components from CEO and suggesting that these compounds might be the most effective ingredients against breast cancer. Besides, we found that CEO treatment suppressed cell proliferation by inducing cell cycle arrest in breast cancer cell lines. Conclusions These findings suggest that CEO inhibit proliferation of breast cancer cell lines through modulating those multi-pathways and multi-targets. The present study not only indicate the therapeutic potential of CEO for breast cancer, but also provide valuable insight into its mechanism of action.

Publisher

Research Square Platform LLC

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