Please use this identifier to cite or link to this item: http://hdl.handle.net/123456789/652
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dc.contributor.authorSingh, Agam Prasad-
dc.date.accessioned2015-09-24T08:33:55Z-
dc.date.available2015-09-24T08:33:55Z-
dc.date.issued2009-09-
dc.identifier.urihttp://hdl.handle.net/123456789/652-
dc.description.abstractAnnually, approximately two million human deaths are caused worldwide by malaria, most of them being children. Plasmodium falciparum is the leading cause of cerebral malaria, the most severe and fatal form of disease. Moreover, the emergence of resistant strains to the existing drugs has worsened the situation. Currently, primaquine is the only drug available for eliminating liver-stage parasites. Because of the emergence of resistant parasite strains, it becomes necessary to find new targets unique to the malaria parasites. In the Plasmodium species, the discovery of a distinct Type-II fatty-acid synthesis pathway has created an opportunity to target this pathway for the development of new inhibitors of malaria parasite growth. The present study explored the growth inhibition potential of triclosan in the case of liver-stage parasites. Liver-stage of Plasmodium is an excellent target for intervention due to very small parasite load as well as possibility of eliminating parasites before it can cause blood-stage infection. Here we report that triclosan inhibits the development of the Plasmodium liver-stage parasites.en_US
dc.publisherInternational Union of Biochemistry and Molecular Biology, Inc.en_US
dc.titleTriclosan inhibit the growth of the late liver-stage of Plasmodiumen_US
dc.contributor.coauthorSurolia, Namita-
dc.contributor.coauthorSurolia, Avadhesha-
dc.keywordMalaria; Liver-stage parasites; Prophylactic drug; Novel antimalarialen_US
dc.journalIUBMB Lifeen_US
dc.volumeno61en_US
dc.issueno9en_US
dc.pages923-928en_US
Appears in Collections:Infectious Disease, Publications

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