Identification of neprilysin as a potential target of arteannuin using computational drug repositioning

Authors

  • Xuan-Yi Ye Lishui University; College of Ecology
  • Qing-Zhi Ling Zhejiang Pharmaceutical College; Department of Traditional Chinese Medicine
  • Shao-Jun Chen Zhejiang Pharmaceutical College; Department of Traditional Chinese Medicine

DOI:

https://doi.org/10.1590/s2175-97902017000216087

Keywords:

Arteannuin/chemical-protein interactome, Computational drug repositioning, Neprilysin/identification, Reverse docking

Abstract

The discovery of arteannuin (qinghaosu) in the 20th Century was a major advance for medicine. Besides functioning as a malaria therapy, arteannuin is a pharmacological agent in a range of other diseases, but its mechanism of action remains obscure. In this study, the reverse docking server PharmMapper was used to identify potential targets of arteannuin. The results were checked using the chemical-protein interactome servers DRAR-CPI and DDI-CPI, and verified by AutoDock Vina. The results showed that neprilysin (also known as CD10), a common acute lymphoblastic leukaemia antigen, was the top disease-related target of arteannuin. The chemical-protein interactome and docking results agreed with those of PharmMapper, further implicating neprilysin as a potential target. Although experimental verification is required, this study provides guidance for future pharmacological investigations into novel clinical applications for arteannuin.

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Published

2017-01-01

Issue

Vol. 53 No. 2 (2017)

Section

Articles

License

All content of the journal, except where identified, is licensed under a Creative Commons attribution-type BY.

The on line journal has open and free access.

How to Cite

Identification of neprilysin as a potential target of arteannuin using computational drug repositioning. (2017). Brazilian Journal of Pharmaceutical Sciences, 53(2), e16087-. https://doi.org/10.1590/s2175-97902017000216087