Frontiers in Pharmacology (Feb 2016)

Metabolomics coupled with multivariate data and pathway analysis on potential biomarkers in cholestasis and intervention effect of Paeonia lactiflora Pall.

  • Xiao eMa,
  • Xiao eMa,
  • Yong-Hui eChi,
  • Ming eNiu,
  • Yun eZhu,
  • Yan-Ling eZhao,
  • Zhe eChen,
  • Zhe eChen,
  • Jia-Bo eWang,
  • Cong-En eZhang,
  • Cong-En eZhang,
  • Jian-Yu eLi,
  • Li-Fu eWang,
  • Man eGong,
  • Shi-Zhang eWei,
  • Shi-Zhang eWei,
  • Chang eChen,
  • Chang eChen,
  • Lu eZhang,
  • Lu eZhang,
  • Ming-Quan eWu,
  • Ming-Quan eWu,
  • Xiao-He eXiao

DOI
https://doi.org/10.3389/fphar.2016.00014
Journal volume & issue
Vol. 7

Abstract

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Background: The dried root of Paeonia lactiflora Pall. (PLP) is a classical Chinese herbal medicine that has been used to treat hepatic disease for thousands of years. Our previous work suggested that PLP can be used to treat hepatitis with severe cholestasis. This study explored the mechanism by which PLP affects ANIT-induced cholestasis in rats using a metabolomics approach.Methods: The effects of PLP on serum indices (TBIL, DBIL, AST, ALT, ALP and TBA) and the histopathology of the liver were analyzed. Moreover, UHPLC-Q-TOF was performed to identify the possible effect of PLP on metabolites. The pathway analysis was conducted to illustrate the pathways and network by which PLP treats cholestasis. Result: High-dose PLP remarkably down-regulated the serum indices and alleviated histological damage to the liver. Metabolomics analyses showed that the therapeutic effect of high-dose PLP is mainly associated with the regulation of several metabolites, such as glycocholic acid, taurocholic acid, glycochenodeoxycholic acid, L(D)-arginine and L-tryptophan. A pathway analysis showed that the metabolites were related to bile acid secretion and amino acid metabolism. In addition, the significant changes in bile acid transporters also indicated that bile acid metabolism might be involved in the therapeutic effect of PLP on cholestasis. Moreover, a principal component analysis indicated that the metabolites in the high-dose PLP group were closer to those of the control, whereas those of the moderate dose or low-dose PLP group were closer to those of the ANIT group. This finding indicated that metabolites may be responsible for the differences between the effects of low-dose and moderate-dose PLP. Conclusions: The therapeutic effect of high-dose PLP on cholestasis is possibly related to regulation of bile acid secretion and amino acid metabolism. Moreover, these findings may help better understand the mechanisms of disease and provide a potential therapy for cholestasis.

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