New developments: chloroquine-resistance in Plasmodium falciparum.

D Warhurst; (2001) New developments: chloroquine-resistance in Plasmodium falciparum. Drug resistance updates, 4 (3). pp. 141-144. ISSN 1368-7646 DOI: 10.1054/drup.2001.0194

Copy

Chloroquine-resistance is associated with higher malaria mortality in children in Africa where the drug is still widely used. In sensitive strains the drug attacks hemoglobin digestion in the lysosome and prevents detoxification of hemin to hemozoin. Reduced drug uptake is responsible for resistance, which is incompletely associated with changes in lysosome membrane protein PGH1. The report discussed here gives evidence for the role of another lysosome membrane protein, PfCRT, where a change from lysine to threonine in a transmembrane domain determines the change to resistance. Other changes in PfCRT, and to some extent change(s) in PGH1, are believed to compensate for loss of fitness of the modified PfCRT.

Item Type	Article
Keywords	Animal, Antimalarials/pharmacology/therapeutic use, Chloroquine/pharmacology/therapeutic use, Drug Resistance/genetics, Human, Malaria, Falciparum/*drug therapy/genetics/metabolism, Animal, Antimalarials, pharmacology, therapeutic use, Chloroquine, pharmacology, therapeutic use, Drug Resistance, genetics, Human, Malaria, Falciparum, drug therapy, genetics, metabolism
ISI	172315400001

Explore Further

Warhurst, D

Dept of Pathogen Molecular Biology (-2019)

Antimicrobial Resistance Centre (AMR)

Drug resistance updates

Full text not available from this repository.

Atom

BibTeX

OpenURL ContextObject in Span

Multiline CSV

OpenURL ContextObject

Dublin Core

MPEG-21 DIDL

EndNote

HTML Citation

JSON

MARC (ASCII)

MARC (ISO 2709)

METS

MODS

RDF+N3

RDF+N-Triples

RDF+XML

RIOXX2 XML

Reference Manager

Refer

Simple Metadata

ASCII Citation

EP3 XML

Export

Downloads