Linkage disequilibrium between two chromosomally 
distinct loci associated with increased resistance to 
chloroquine in Plasmodium falciparum

DURAISINGH MT.; VON SEIDLEIN L.; JEPSON A.; JONES P.; SAMBOU I.; PINDER M.; WARHURST DC.

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Linkage disequilibrium between two chromosomally distinct loci associated with increased resistance to chloroquine in Plasmodium falciparum

DURAISINGH MT., VON SEIDLEIN L., JEPSON A., JONES P., SAMBOU I., PINDER M., WARHURST DC.

<jats:p>Chloroquine-resistance in <jats:italic>Plasmodium falciparum</jats:italic> is associated with polymorphisms in a locus on or near the <jats:italic>cg2</jats:italic> gene on chromosome 7, and in the <jats:italic>pfmdr1</jats:italic> gene on chromosome 5. In this study we typed <jats:italic>P. falciparum</jats:italic> DNA from uncomplicated malaria cases in The Gambia in 1990, 1995 and 1996 for size polymorphism in the omega repeat of <jats:italic>cg2</jats:italic>, for sequence polymorphisms in <jats:italic>pfmdr1</jats:italic> at codons 86 and 184, in <jats:italic>dhfr</jats:italic> at codon 108 and in the <jats:italic>msp2</jats:italic> gene. Chloroquine sensitivity tests were conducted <jats:italic>in vitro</jats:italic>. A significant but incomplete association was found between the presence of the <jats:italic>cg2</jats:italic> Dd2-like omega repeat size polymorphism and <jats:italic>in vitro</jats:italic> resistance, and between the tyr-86 allele of <jats:italic>pfmdr1</jats:italic> and <jats:italic>in vitro</jats:italic> resistance. Furthermore there was strong linkage disequilibrium between the <jats:italic>pfmdr1</jats:italic> asn-86 allele and the <jats:italic>cg2</jats:italic> not Dd2-like omega repeat allele located on different chromosomes. In contrast, no linkage disequilibrium was found between these alleles and either the <jats:italic>dhfr</jats:italic> ser-108 allele or the <jats:italic>msp2</jats:italic> IC sequence polymorphism. No significant linkage was measured between <jats:italic>pfmdr1</jats:italic> asn-86 and phe-184 although these loci are separated only by 296 base pairs. Our results suggest that genetic elements linked to the <jats:italic>cg2</jats:italic> and the <jats:italic>pfmdr1</jats:italic> genes are important determinants of chloroquine resistance. It can be concluded that the observed linkage disequilibrium is maintained epistatically through selection by chloroquine.</jats:p>

Original publication

DOI

10.1017/s0031182099006022

Type

Journal

Parasitology

Publisher

Cambridge University Press (CUP)

Publication Date

07/2000

Volume

121

Pages

1 - 7