The antihyperuricemic and nephroprotective effect of puerarin by reducing uric acid level and exerting anti‐inflammatory activity

Author:

Wang Muxuan12,Zhao Yong3,Chen Nan2,Wang Yanao2,Guo Xu2,Li Ningyang4,Liu Haoran5,Sun Hui4,Liu Chao26ORCID,Liao Zhixin1

Affiliation:

1. Department of Pharmaceutical Engineering School of Chemistry and Chemical Engineering, and Jiangsu Province Hi‐Tech Key Laboratory for Biomedical Research, Southeast University Nanjing China

2. Key Laboratory of Novel Food Resources Processing, Ministry of Agriculture and Rural Affairs/Key Laboratory of Agro‐Products Processing Technology of Shandong Province Institute of Food & Nutrition Science and Technology, Shandong Academy of Agricultural Sciences Jinan China

3. The Agricultural Exchange and Cooperation Center of Shandong Province Jinan China

4. Shandong Marine Food Engineering Technology Research Center College of Food Science and Engineering, Ocean University of China Qingdao China

5. Shandong Meiguolai Food Co., Ltd Zaozhuang China

6. Shandong Aojing Biotechnology Co., Ltd Jining China

Abstract

AbstractHyperuricemia (HUA) is a common metabolic disease and kidney injury is one of its main complications. As a typical natural flavonoid, puerarin (PEA) has a range of pharmacological activity but the antihyperuricemic mechanism of PEA has not been reported. Herein, the inhibitory activity of PEA against xanthine oxidase (XOD) was evaluated by in vitro enzymatic reaction, and kinetic analysis, the antihyperuricemic activity, and nephroprotective effect of PEA were studied in HUA mice. The enzymatic reaction showed that the inhibitory effect of PEA (half maximal inhibitory concentration [IC50] = 4.39 µmol/L) on XOD was at the same level as allopurinol (IC50 = 4.05 µmol/L), and kinetic analysis indicated that PEA was a mixed competitive inhibitor. In vivo studies demonstrated that PEA exhibited excellent antihyperuricemic activity by inhibiting XOD and urate transporter 1 (URAT1), to reduce uric acid level. At the same time, PEA reduced the level of inflammatory cytokines and exerted significant nephroprotective effect through anti‐inflammatory activity. Molecular docking indicated that PEA closely bind to both XOD and URAT1, which had the potential to become an inhibitor of XOD and URAT1. In summary, PEA has important application value in developing novel functional food and medicine for the treatment of HUA and its complications.

Publisher

Wiley

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