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Antimalarial Drugs and their Useful Therapeutic Lives: Rational Drug Design Lessons from Pleiotropic Action of Quinolines and Artemisinins

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dc.contributor.authorMuregi, Francis W
dc.date.accessioned2024-07-25T09:32:30Z
dc.date.available2024-07-25T09:32:30Z
dc.date.issued2010
dc.description.abstractEfforts to develop an effective malarial vaccine are yet to be successful and thus chemotherapy remains the mainstay of malaria control strategy. Unfortunately, Plasmodium falciparum, the parasite that causes about 90% of all global malaria cases is increasingly becoming resistant to classical antimalarials, necessitating a search for new chemotherapeutics preferably with novel modes of action. Today, rational drug discovery strategy is gaining new impetus as knowledge of malaria parasite biology expands, aided by the parasite genome database and improved bioinformatics tools. Drug development is a laborious, time consuming and costly process, and thus the “useful therapeutic lives” (UTLs) of new drugs should be commensurate with the resources invested in their development. Historical evidence on development and evolution of resistance to classical antimalarial drugs shows that the mode of action of a drug influences its UTL. Drugs that target single and specific targets such as antimalarial antifolates and atovaquone (ATQ) are rendered ineffective within a short time of their clinical use, unlike drugs with pleiotropic action such as chloroquine (CQ) and artemisinins (ART) with long UTLs. Unfortunately, almost all new targets currently being explored for development of novel drugs belong to the “specific target” other than the “multiple target” category, and is plausible that such drugs will have short UTLs. This review relates the pleiotropic action of CQ and ART with their long UTLs, and discusses their relevance in rational drug development strategies. Novel targets with potential to yield drugs with long UTLs are also explored.
dc.identifier.citationJOUR Muregi, Francis 2010/10/01 280 316 Antimalarial Drugs and their Useful Therapeutic Lives: Rational Drug Design Lessons from Pleiotropic Action of Quinolines and Artemisinins 7 10.2174/157016310793360693 Current drug discovery technologies
dc.identifier.issn1570-1638
dc.identifier.urihttps://erepository.mku.ac.ke/handle/123456789/6140
dc.language.isoen
dc.publisherBentham Science Publishers
dc.subject: Antimalarials design
dc.subjectantimalarial resistance
dc.subjectantimalarial targets
dc.subjectmalaria chemotherapy
dc.subjectPlasmodium falciparum
dc.subjectuseful therapeutic life
dc.subjectQuinolines
dc.subjectArtemisinins
dc.subjectmalarial vaccine
dc.subjectchemotherapy
dc.subjectantimalarial antifolates
dc.subjectatovaquone
dc.subjectchloroquine
dc.subjectprotozoal parasite
dc.subjectP. vivax
dc.subjectP. ovale
dc.subjectP. malariae
dc.subjectMedicines for Malaria Venture
dc.subjectproguanil
dc.subjectsulfadoxine/ pyrimethamine (Fansidar)
dc.subjectPaludrine
dc.subjectpyrimethamine
dc.subjectDaraprim
dc.subjectSN10275
dc.subjectmefloquine
dc.subjectdihydroartemisinin
dc.subjectlumefantrine
dc.subject4-aminoquinolines
dc.subjectarylaminoalcohols quinine
dc.subjecthalofantrine
dc.subjecthaemozoin
dc.subjectmembrane-associated FPIX
dc.subjectp-hydroxyanilino aromatic ring
dc.subjectAMQ-protein complexes
dc.subjectagranulocytosis
dc.subjectprophylaxis
dc.subjectpyronaridine-artesunate combination
dc.subjectartemether-lumefantrine
dc.subjectBis(quinolyl)-piperazines
dc.subjectpiperaquine
dc.subjectCQ-resistant malaria
dc.subjectintraerythrocytic parasite
dc.subjectiron II ferriprotoporphyrin IX
dc.subjectSynthetic Peroxides
dc.subjectHydroxynaphthoquinones
dc.subjectPyrimidine biosynthetic enzymes
dc.subjectshikimate pathway
dc.subjectErythrocyte Membrane Proteins
dc.titleAntimalarial Drugs and their Useful Therapeutic Lives: Rational Drug Design Lessons from Pleiotropic Action of Quinolines and Artemisinins
dc.typeArticle
dspace.entity.typePublication

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