Author
Listed:
- Julie A. Frearson
(Drug Discovery Unit)
- Stephen Brand
(Drug Discovery Unit)
- Stuart P. McElroy
(Drug Discovery Unit)
- Laura A. T. Cleghorn
(Drug Discovery Unit)
- Ondrej Smid
(Drug Discovery Unit)
- Laste Stojanovski
(Drug Discovery Unit)
- Helen P. Price
(Centre for Immunology and Infection, University of York, Heslington, York YO10 5YW, UK)
- M. Lucia S. Guther
(Drug Discovery Unit)
- Leah S. Torrie
(Drug Discovery Unit)
- David A. Robinson
(Drug Discovery Unit)
- Irene Hallyburton
(Drug Discovery Unit)
- Chidochangu P. Mpamhanga
(Drug Discovery Unit)
- James A. Brannigan
(Structural Biology Laboratory)
- Anthony J. Wilkinson
(Structural Biology Laboratory)
- Michael Hodgkinson
(Centre for Immunology and Infection, University of York, Heslington, York YO10 5YW, UK)
- Raymond Hui
(Structural Genomics Consortium, University of Toronto, MaRS South Tower, 7th Floor, 101 College Street, Toronto, Ontario M5G 1L7, Canada)
- Wei Qiu
(Structural Genomics Consortium, University of Toronto, MaRS South Tower, 7th Floor, 101 College Street, Toronto, Ontario M5G 1L7, Canada)
- Olawale G. Raimi
(College of Life Sciences, University of Dundee, Dundee DD1 5EH, UK)
- Daan M. F. van Aalten
(College of Life Sciences, University of Dundee, Dundee DD1 5EH, UK)
- Ruth Brenk
(Drug Discovery Unit)
- Ian H. Gilbert
(Drug Discovery Unit)
- Kevin D. Read
(Drug Discovery Unit)
- Alan H. Fairlamb
(Drug Discovery Unit)
- Michael A. J. Ferguson
(Drug Discovery Unit)
- Deborah F. Smith
(Centre for Immunology and Infection, University of York, Heslington, York YO10 5YW, UK)
- Paul G. Wyatt
(Drug Discovery Unit)
Abstract
African sleeping sickness or human African trypanosomiasis, caused by Trypanosoma brucei spp., is responsible for ∼30,000 deaths each year. Available treatments for this disease are poor, with unacceptable efficacy and safety profiles, particularly in the late stage of the disease when the parasite has infected the central nervous system. Here we report the validation of a molecular target and the discovery of associated lead compounds with the potential to address this lack of suitable treatments. Inhibition of this target—T. brucei N-myristoyltransferase—leads to rapid killing of trypanosomes both in vitro and in vivo and cures trypanosomiasis in mice. These high-affinity inhibitors bind into the peptide substrate pocket of the enzyme and inhibit protein N-myristoylation in trypanosomes. The compounds identified have promising pharmaceutical properties and represent an opportunity to develop oral drugs to treat this devastating disease. Our studies validate T. brucei N-myristoyltransferase as a promising therapeutic target for human African trypanosomiasis.
Suggested Citation
Julie A. Frearson & Stephen Brand & Stuart P. McElroy & Laura A. T. Cleghorn & Ondrej Smid & Laste Stojanovski & Helen P. Price & M. Lucia S. Guther & Leah S. Torrie & David A. Robinson & Irene Hallyb, 2010.
"N-myristoyltransferase inhibitors as new leads to treat sleeping sickness,"
Nature, Nature, vol. 464(7289), pages 728-732, April.
Handle:
RePEc:nat:nature:v:464:y:2010:i:7289:d:10.1038_nature08893
DOI: 10.1038/nature08893
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Cited by:
- Mutian Jia & Yuanyuan Wang & Jie Wang & Danhui Qin & Mengge Wang & Li Chai & Yue Fu & Chunyuan Zhao & Chengjiang Gao & Jihui Jia & Wei Zhao, 2023.
"Myristic acid as a checkpoint to regulate STING-dependent autophagy and interferon responses by promoting N-myristoylation,"
Nature Communications, Nature, vol. 14(1), pages 1-12, December.
- Aditi Mukherjee & Zakir Hossain & Esteban Erben & Shuai Ma & Jun Yong Choi & Hee-Sook Kim, 2023.
"Identification of a small-molecule inhibitor that selectively blocks DNA-binding by Trypanosoma brucei replication protein A1,"
Nature Communications, Nature, vol. 14(1), pages 1-19, December.
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