Drug repurposing and human parasitic protozoan diseases

•Anti-protozoan drug discovery is challenging, time consuming and expensive.•Drug repurposing has historically played a role in anti-protozoan drug discovery.•Drug repurposing can result in significant time and cost savings.•Here we review drug repurposing for major human protozoan diseases. Parasit...

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Bibliographic Details
Published in:International journal for parasitology -- drugs and drug resistance 2014-08, Vol.4 (2), p.95-111
Main Authors: Andrews, Katherine T., Fisher, Gillian, Skinner-Adams, Tina S.
Format: Article
Language:English
Subjects:
Antiparasitic
Cryptosporidium
Drug repurposing
Invited Review
Leishmaniasis
Malaria
Toxoplasmosis
Trypanosomiasis
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Summary:•Anti-protozoan drug discovery is challenging, time consuming and expensive.•Drug repurposing has historically played a role in anti-protozoan drug discovery.•Drug repurposing can result in significant time and cost savings.•Here we review drug repurposing for major human protozoan diseases. Parasitic diseases have an enormous health, social and economic impact and are a particular problem in tropical regions of the world. Diseases caused by protozoa and helminths, such as malaria and schistosomiasis, are the cause of most parasite related morbidity and mortality, with an estimated 1.1million combined deaths annually. The global burden of these diseases is exacerbated by the lack of licensed vaccines, making safe and effective drugs vital to their prevention and treatment. Unfortunately, where drugs are available, their usefulness is being increasingly threatened by parasite drug resistance. The need for new drugs drives antiparasitic drug discovery research globally and requires a range of innovative strategies to ensure a sustainable pipeline of lead compounds. In this review we discuss one of these approaches, drug repurposing or repositioning, with a focus on major human parasitic protozoan diseases such as malaria, trypanosomiasis, toxoplasmosis, cryptosporidiosis and leishmaniasis.
ISSN:2211-3207
2211-3207
DOI:10.1016/j.ijpddr.2014.02.002