[Efficacy and mechanism of new resource medicinal materia Moringa oleifera leaves against hyperlipidemia]

Zi-Jun Sha; Cai-Feng Li; Shi-Huan Tang; Hong-Jun Yang; Yi Zhang; Zhi-Yong Li; Bin Yang

doi:10.19540/j.cnki.cjcmm.20210309.401

[Efficacy and mechanism of new resource medicinal materia Moringa oleifera leaves against hyperlipidemia]

Zhongguo Zhong Yao Za Zhi. 2021 Jul;46(14):3465-3477. doi: 10.19540/j.cnki.cjcmm.20210309.401.

[Article in Chinese]

Authors

Zi-Jun Sha¹, Cai-Feng Li², Shi-Huan Tang³, Hong-Jun Yang³, Yi Zhang³, Zhi-Yong Li⁴, Bin Yang³

Affiliations

¹ School of Pharmacy,Minzu University of China Beijing 100081,China Institute of Chinese Materia Medica,China Academy of Chinese Medical Sciences Beijing 100700,China.
² Academician Workstation of Jiangxi University of Traditional Chinese Medicine Nanchang 330004,China National Resource Center for Chinese Materia Medica,China Academy of Chinese Medical Sciences Beijing 100700,China.
³ Institute of Chinese Materia Medica,China Academy of Chinese Medical Sciences Beijing 100700,China.
⁴ School of Pharmacy,Minzu University of China Beijing 100081,China Collaborative Innovation Center for the Development of New Chinese Medicine Resources in Yunnan Kunming 650051,China Faculty of Life Science and Technology,Kunming University of Science and Technology Kunming 650504,China.

PMID: 34402268
DOI: 10.19540/j.cnki.cjcmm.20210309.401

Abstract

High fat diet induced hyperlipidemia hamster model was used to explore the anti-hyperlipidemia effect of water extract of Moringa oleifera leaves( WEMOL). On this basis,the possible action mechanism was predicted by network pharmacology. Golden hamsters were randomly divided into normal diet group( NFD),high-fat diet group( HFD),simvastatin group,high dose group of WEMOL( HIWEMOL) and low dose group of WEMOL( LOWEMOL). The model was administered simultaneously for 66 days,during which the body weight changes of hamsters were recorded. At the end of the experiment,serum lipid level and serum transaminase level of golden hamsters in each group were detected,and the pathological changes of liver were observed by hematoxylin-eosin( HE) staining. The results showed that WEMOL could significantly decrease the serum total cholesterol( TC),total triglyceride( TG),low density lipoprotein cholesterol( LDL-c) levels,and reduce the lipid deposition in liver tissue,thus improving the hyperlipidemia of golden hamsters. According to the prediction of network pharmacology,219 targets of potential active components of M.oleifera leaves and 185 targets of water-soluble potential active components of M. oleifera leaves for the treatment of hyperlipidemia were obtained separately. The MCODE analysis was performed on the PPI network of 219 targets and 185 targets obtained above and got five and four clusters respectively. The signaling pathway analysis of clusters showed that among the common pathways,nonalcoholic fatty liver,insulin resistance,MAPK signaling pathway,estrogen signaling pathway,cell apoptosis and HIF-1 signaling pathway were associated with hyperlipidemia. In addition,the potential active components of M. oleifera leaves could also inhibit the metabolic inflammation of hyperlipidemia by modulating complement and coagulation cascades signaling pathway,and GSK3 B,F2,AKT1,RELA,SERPINE1 might be the key targets. The water-soluble potential active components of M. oliefera leaves could modulate lipid metabolism by modulating AMPK signaling pathway and JAK-STAT signaling pathway,with PIK3 CB,PIK3 CA,CASP3,AKT1 and BCL2 as the key targets. These results suggested that WEMOL had anti hyperlipidemia effect,and its mechanism might be related to the protein expression regulation of lipid metabolism,nonalcoholic fatty liver disease and atherosclerosis related signaling pathways.

Keywords: Moringa oleifera leaves; hyperlipidemia; lipid-lowering mechanism; network pharmacology.

MeSH terms

Animals
Cricetinae
Diet, High-Fat
Glycogen Synthase Kinase 3
Hyperlipidemias* / drug therapy
Liver
Moringa oleifera*
Plant Leaves

Substances

Glycogen Synthase Kinase 3