Publication:
Novel Rational Drug Design Strategies with Potential to Revolutionize Malaria Chemotherapy

Simple item page
dc.contributor.authorA Ishih
dc.contributor.authorKirira, Peter G
dc.contributor.authorMuregi, Francis W
dc.date.accessioned2024-07-25T09:23:30Z
dc.date.available2024-07-25T09:23:30Z
dc.date.issued2011
dc.description.abstractEfforts to develop an effective malaria vaccine are yet to be successful and thus chemotherapy remains the mainstay of malaria control strategy. Plasmodium falciparum, the parasite that causes about 90% of all global malaria cases is increasingly becoming resistant to most antimalarial drugs in clinical use. This dire situation is aggravated by reports from Southeast Asia, of the parasite becoming resistant to the "magic bullet" artemisinins, the last line of defense in malaria chemotherapy. Drug development is a laborious and time consuming process, and thus antimalarial drug discovery approaches currently being deployed largely include optimization of therapy with available drugs--including combination therapy and developing analogues of the existing drugs. However, the latter strategy may be hampered by crossresistance, since agents that are closely related chemically may share similar mechanisms of action and/or targets. This may render new drugs ineffective even before they are brought to clinical use. Evaluation of drug-resistance reversers (chemosensitizers) against quinoline-based drugs such as chloroquine and mefloquine is another approach that is being explored. Recently, evaluation of new chemotherapeutic targets is gaining new impetus as knowledge of malaria parasite biology expands. Also, single but hybrid molecules with dual functionality and/or targets have been developed through rational drug design approach, termed as "covalent bitherapy". Since desperate times call for radical measures, this review aims to explore novel rational drug-design strategies potentially capable of revolutionizing malaria therapy. We thus explore malaria apoptosis machinery as a novel drug target, and also discuss the potential of hybrid molecules as well as prodrugs and double prodrugs in malaria chemotherapy.
dc.identifier.citationMuregi, Francis Kirira, Peter Ishih, A 2011/01/01 113 43 Novel Rational Drug Design Strategies with Potential to Revolutionize Malaria Chemotherapy 18 10.2174/092986711793979742 Current medicinal chemistry
dc.identifier.issn0929-8673
dc.identifier.urihttps://erepository.mku.ac.ke/handle/123456789/6139
dc.language.isoen
dc.publisherBentham Science Publishers
dc.subjectAntimalarial drugs
dc.subjectapoptosis
dc.subjecthybrid drugs
dc.subjectPlasmodium falciparum
dc.subjectprodrugs
dc.subjecttopoisomerases
dc.subjectRational Drug
dc.subjectChemotherapy
dc.subjectprotozoal parasite
dc.subjectPlasmodium
dc.subjectmalaria
dc.subjectchloroquine
dc.subjectantifolates
dc.subjectWorld Health Organization
dc.subjectartesunate-sulfadoxine pyrimethamine
dc.subjectchemosensitizers
dc.subjectbioinformatics tools
dc.subjectcysteine
dc.subjectaspartic proteases
dc.subjecthaemoglobin metabolism
dc.subjectintraerythrocytic
dc.subjectplasmepsins
dc.subjectpeptidomimetic compounds
dc.subjectProtease inhibitors
dc.subjectpurine salvage
dc.subjectpyrimidine biosynthetic
dc.subjectdehydrogenase
dc.subjecteukaryotes
dc.subjectneurological disorders
dc.subjectcarboxy terminal
dc.subjectRNA polymerase II
dc.subjectplasmodial CDK inhibitors
dc.subjectGlutathione
dc.subjectApicoplast
dc.subjectcytosol
dc.subjectfungi
dc.subjectTriclosan
dc.subjecthaemoglobin
dc.subjecttrophozoite
dc.subjectciprofloxacin
dc.subjectschizogony
dc.subjectDNA
dc.subjectprosthetic groups
dc.subjectisoforms
dc.subjectlipoic acid
dc.subjectDepolarization
dc.subjectmitochondrial membrane
dc.subjectcytochrome
dc.subjectcovalent bitherapy
dc.subjectanticancer agents
dc.subjecthomeostatic functions
dc.subjectdysfunctional DNA
dc.subjectcell-shrinkage
dc.subjectnecrosis
dc.subjectEntamoeba histolytica
dc.subjectDictyostelium discoideum
dc.subjectintracellular K+
dc.subjectsodium nitroprusside
dc.subjectmitochondrial dysfunction
dc.subjectisolates
dc.subjectcytoplasmatic vacuolization
dc.subjectsynchrony
dc.subjectcell shrinkage
dc.subjectMosquitoes
dc.subjectvertebrate host
dc.subjectzygote
dc.subjectookinete
dc.subjectsporogonic stage
dc.subjectdensity
dc.subjectorthologues
dc.subjectimmune system
dc.subjectmembrane blebbing
dc.subjectnovel drug
dc.subjectcalcium pools
dc.subjecttransferrin receptor (TfR)
dc.subjectintraerythrocytic parasites
dc.subjectpromyelocytic leukemia
dc.subjectReduction
dc.subjectcell-signaling enzymes
dc.subjectADP-ribosylation
dc.subjectDNA Topoisomerases
dc.subjectsupecoils
dc.subjectATP
dc.subjectcofactor
dc.subjectpadophyllotoxin
dc.subjectEpipodophyllotoxins
dc.subjectsarcoma
dc.subjecttesticular cancer
dc.subjectacute lymphocytic leukemia
dc.subjectsmall-cell lung cancer
dc.subjectInhibitors
dc.subjectanthracycline
dc.subjectpoisons
dc.subjecthybrid molecules
dc.subjectxenobiotic detoxification
dc.subjectvasodilators
dc.subjectpenfluridol
dc.subjectarchaebacterial topoisomerase
dc.subjectalkylating agent
dc.subjectheterocycle
dc.subjectconjugated
dc.subjectdrug's availability
dc.subjectverapamil
dc.subjectantiplasmodial activity
dc.subjectrational drug design
dc.subjecttypical dual drug
dc.subjectelucidation of drugs
dc.subjectbioactive drug
dc.subjectNovel Rational Drug Design Strategies with Potential to Revolutionize Malaria Chemotherapy
dc.titleNovel Rational Drug Design Strategies with Potential to Revolutionize Malaria Chemotherapy
dc.typeArticle
dspace.entity.typePublication

Files

License bundle

Now showing 1 - 1 of 1
Thumbnail Image
Name:
license.txt
Size:
1.71 KB
Format:
Item-specific license agreed upon to submission
Description:
Download

Collections

Health Sciences