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Elucidating antimalarial drug targets/mode-of-action by application of system biology technologies

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dc.contributor.author Becker, J
dc.contributor.author Mtwisha, L
dc.contributor.author Crampton, B
dc.contributor.author Mancama, Dalubuhle T
dc.date.accessioned 2009-01-19T13:36:24Z
dc.date.available 2009-01-19T13:36:24Z
dc.date.issued 2008-11
dc.identifier.citation Becker, J, Mtwisha, L, Crampton, B et al. 2008. Elucidating antimalarial drug targets/mode-of-action by application of system biology technologies. Science real and relevant: 2nd CSIR Biennial Conference, CSIR International Convention Centre Pretoria, 17 & 18 November 2008, pp 1 en
dc.identifier.uri http://hdl.handle.net/10204/2842
dc.description Science real and relevant: 2nd CSIR Biennial Conference, CSIR International Convention Centre Pretoria, 17 & 18 November 2008 en
dc.description.abstract Malaria is one of the world's most important tropical diseases, killing more than a million of an estimated 300-500 million infected people per annum. The species responsible for the most fatalities amongst the genus is Plasmodium falsiparum. Eradication efforts are hampered by two major drawbacks-the absence of an effective vaccine coupled with the widespread occurrence of drug-resistant strains to frontline antimalarials and, of late, the emergence of resistance to current antimalarials of choice. In this regard, the researchers chose the polymine metabolic pathway in P. falciparum as a proof of concept project, to validate the pathway as a drug target and elucidate the (MoA) of cyclohexylamine in P. falciparum 3D7. Drug effects were examined through morphological characterisation of the parasite's life cycle, as well as transcriptomic and proteomic analyses. en
dc.language.iso en en
dc.publisher CSIR en
dc.subject Malaria en
dc.subject Antimalarial drug targets en
dc.subject System biology technology en
dc.subject Polyamine metabolic en
dc.title Elucidating antimalarial drug targets/mode-of-action by application of system biology technologies en
dc.type Conference Presentation en
dc.identifier.apacitation Becker, J., Mtwisha, L., Crampton, B., & Mancama, D. T. (2008). Elucidating antimalarial drug targets/mode-of-action by application of system biology technologies. CSIR. http://hdl.handle.net/10204/2842 en_ZA
dc.identifier.chicagocitation Becker, J, L Mtwisha, B Crampton, and Dalubuhle T Mancama. "Elucidating antimalarial drug targets/mode-of-action by application of system biology technologies." (2008): http://hdl.handle.net/10204/2842 en_ZA
dc.identifier.vancouvercitation Becker J, Mtwisha L, Crampton B, Mancama DT, Elucidating antimalarial drug targets/mode-of-action by application of system biology technologies; CSIR; 2008. http://hdl.handle.net/10204/2842 . en_ZA
dc.identifier.ris TY - Conference Presentation AU - Becker, J AU - Mtwisha, L AU - Crampton, B AU - Mancama, Dalubuhle T AB - Malaria is one of the world's most important tropical diseases, killing more than a million of an estimated 300-500 million infected people per annum. The species responsible for the most fatalities amongst the genus is Plasmodium falsiparum. Eradication efforts are hampered by two major drawbacks-the absence of an effective vaccine coupled with the widespread occurrence of drug-resistant strains to frontline antimalarials and, of late, the emergence of resistance to current antimalarials of choice. In this regard, the researchers chose the polymine metabolic pathway in P. falciparum as a proof of concept project, to validate the pathway as a drug target and elucidate the (MoA) of cyclohexylamine in P. falciparum 3D7. Drug effects were examined through morphological characterisation of the parasite's life cycle, as well as transcriptomic and proteomic analyses. DA - 2008-11 DB - ResearchSpace DP - CSIR KW - Malaria KW - Antimalarial drug targets KW - System biology technology KW - Polyamine metabolic LK - https://researchspace.csir.co.za PY - 2008 T1 - Elucidating antimalarial drug targets/mode-of-action by application of system biology technologies TI - Elucidating antimalarial drug targets/mode-of-action by application of system biology technologies UR - http://hdl.handle.net/10204/2842 ER - en_ZA


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