WEI Zi-yi, XU Wen-juan, DONG Jiao-jiao, LIU Jie, JIA Zhi-xin, CHEN Yi-jun, WANG Ming-xia, YANG Jiao, XIAO Hong-bin. Hydroxysafflor yellow A repairing the metabolic disturbances of early atherosclerosis based on fatty acid profilingJ. Acta Pharmaceutica Sinica, 2018,53(10): 1680-1688. doi: 10.16438/j.0513-4870.2018-0409
Citation: WEI Zi-yi, XU Wen-juan, DONG Jiao-jiao, LIU Jie, JIA Zhi-xin, CHEN Yi-jun, WANG Ming-xia, YANG Jiao, XIAO Hong-bin. Hydroxysafflor yellow A repairing the metabolic disturbances of early atherosclerosis based on fatty acid profilingJ. Acta Pharmaceutica Sinica, 2018,53(10): 1680-1688. doi: 10.16438/j.0513-4870.2018-0409

Hydroxysafflor yellow A repairing the metabolic disturbances of early atherosclerosis based on fatty acid profiling

  • Atherosclerosis (AS) is a complex metabolic syndrome that seriously harms human health, and its occurrence and development are directly related to the metabolic disturbances of free fatty acids (FFA). In this study, macrophage-derived foam cells were established as the model of early AS. Therefore, the metabolic disturbances of FFA in ox-LDL induced foamy macrophages were analyzed using target metabolomics. Then the effect of hydroxysafflor yellow A (HSYA) on regulating FFA was also explored. The quantitative analysis of 27 fatty acids was obtained within 20 min based on dynamic MRM mode. Thirteen metabolic biomarkers of macrophage-derived foam cells were identified using multivariate statistical analysis. It was found that upregulation of total SFA and downregulation of C12:0, C14:0, C18:1, total MUFA were the typical metabolic features in macrophage-derived foam cells. Furthermore, HSYA displayed obvious repairing effect on C12:0, C14:0 and C18:1, which were involved in de novo fatty acid biosynthesis pathway. Oleoyl-(acyl-carrier-protein) hydrolase (OLAH), as the key enzyme in de novo fatty acid biosynthesis pathway, may be a drug target of HSYA.
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