4.6 Article

PDK1/Akt/PDE4D axis identified as a target for asthma remedy synergistic with β2AR agonists by a natural agent arctigenin

期刊

ALLERGY
卷 70, 期 12, 页码 1622-1632

出版社

WILEY
DOI: 10.1111/all.12763

关键词

arctigenin; chemical proteomics; PDK1; PDK1/Akt/PDE4D axis; beta(2)AR agonists

资金

  1. National Natural Science Foundation of China [81430095, 81173638, 81373506]
  2. State Key Laboratory of Natural and Biomimetic Drugs [K20140203]
  3. Specialized Research Fund for Doctor Program of Higher Education of China [20120031110042]
  4. Key Program of Natural Science Foundation of Tianjin, China [13JCZDJC31400]

向作者/读者索取更多资源

Background: Asthma is a heterogenetic disorder characterized by chronic inflammation with variable airflow obstruction and airway hyper-responsiveness. As the most potent and popular bronchodilators, beta(2) adrenergic receptor (beta(2)AR) agonists bind to the beta(2)ARs that are coupled via a stimulatory G protein to adenylyl cyclase, thereby improving cAMP accumulation and resulting in airway smooth muscle relaxation. We previously demonstrated arctigenin had a synergistic function with the beta(2)AR agonist, but the target for this remained elusive. Method: Chemical proteomics capturing was used to enrich and uncover the target of arctigenin in human bronchial smooth muscle cells, and reverse docking and molecular dynamic stimulation were performed to evaluate the binding of arctigenin and its target. In vitro enzyme activities and protein levels were demonstrated with special kits and Western blotting. Finally, guinea pig tracheal muscle segregation and ex vivo function were analysed. Results: Arctigenin bound to PDK1 with an ideal binding free energy-25.45 kcal/mol and inhibited PDK1 kinase activity without changing its protein level. Additionally, arctigenin reduced PKB/Akt-induced phosphorylation of PDE4D, which was first identified in this study. Attenuation of PDE4D resulted in cAMP accumulation in human bronchial smooth muscle. The inhibition of PDK1 showed a synergistic function with beta(2)AR agonists and relaxed the constriction of segregated guinea pig tracheal muscle. Conclusions: The PDK1/Akt/PDE4D axis serves as a novel asthma target, which may benefit airflow obstruction.

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