Genetic diversity of Plasmodium falciparum parasites from Kenya is not affected by antifolate drug selection

A. M. Nzila; E. K. Mberu; E. Nduati; A. Ross; W. M. Watkins; C. H. Sibley

doi:10.1016/S0020-7519(02)00164-9

Genetic diversity of Plasmodium falciparum parasites from Kenya is not affected by antifolate drug selection

A. M. Nzila^*, E. K. Mberu, E. Nduati, A. Ross, W. M. Watkins, C. H. Sibley

^*Corresponding author for this work

Research output: Contribution to journal › Article › peer-review

14 Scopus citations

Abstract

The genotypes of merozoite surface protein-1, merozoite surface protein-2 and glutamine rich protein are frequently used to distinguish recrudescence from reinfection when parasitaemia reappears after antimalarial drug treatment. However, none of the previous reports has clearly assessed the change of genetic diversity following drug treatment. In the present study, we have assessed the impact of pyrimethamine/sulfadoxine and chlorproguanil/dapsone on the genetic diversity of isolates and the multiplicity of infection in patient isolates from Kilifi, Kenya. We have analysed the length polymorphism of merozoite surface protein-1, merozoite surface protein-2 and glutamine rich protein and the data clearly show that treatment with pyrimethamine/sulfadoxine and chlorproguanil/dapsone did not change the multiplicity of infection found in patients, in contrast to the selection that these drugs exert on the genes encoded by the target enzymes. In addition, we report that children of less than 2 years tend to have fewer numbers of clones per isolate when compared with older children. Overall, this study shows that the selection for genes that confer drug resistance is not a factor in reducing the genetic diversity of parasite clones in a patient.

Original language	English
Pages (from-to)	1469-1476
Number of pages	8
Journal	International Journal for Parasitology
Volume	32
Issue number	12
DOIs	https://doi.org/10.1016/S0020-7519(02)00164-9
State	Published - Nov 2002
Externally published	Yes

Bibliographical note

Funding Information:
We thank the director of Kenya Medical Research Institute for permission to publish these data. This work was supported by the Wellcome Trust of Great Britain (grant ref. Nos. 045010 and 056769), the UNDP/World Bank/WHO Special program for Research and Training in Tropical Diseases (980369) and NIH grant AI 42321 to CHS. A.M.N., E.K.M., E.N., A.R. and W.M.W. are grateful to the Wellcome Trust for personal support.

Keywords

Antifolates
Malaria genetic diversity
Plasmodium falciparum

ASJC Scopus subject areas

Parasitology
Infectious Diseases

UN SDGs

This output contributes to the following UN Sustainable Development Goals (SDGs)

Access to Document

10.1016/S0020-7519(02)00164-9

Cite this

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title = "Genetic diversity of Plasmodium falciparum parasites from Kenya is not affected by antifolate drug selection",

abstract = "The genotypes of merozoite surface protein-1, merozoite surface protein-2 and glutamine rich protein are frequently used to distinguish recrudescence from reinfection when parasitaemia reappears after antimalarial drug treatment. However, none of the previous reports has clearly assessed the change of genetic diversity following drug treatment. In the present study, we have assessed the impact of pyrimethamine/sulfadoxine and chlorproguanil/dapsone on the genetic diversity of isolates and the multiplicity of infection in patient isolates from Kilifi, Kenya. We have analysed the length polymorphism of merozoite surface protein-1, merozoite surface protein-2 and glutamine rich protein and the data clearly show that treatment with pyrimethamine/sulfadoxine and chlorproguanil/dapsone did not change the multiplicity of infection found in patients, in contrast to the selection that these drugs exert on the genes encoded by the target enzymes. In addition, we report that children of less than 2 years tend to have fewer numbers of clones per isolate when compared with older children. Overall, this study shows that the selection for genes that confer drug resistance is not a factor in reducing the genetic diversity of parasite clones in a patient.",

keywords = "Antifolates, Malaria genetic diversity, Plasmodium falciparum",

author = "Nzila, \{A. M.\} and Mberu, \{E. K.\} and E. Nduati and A. Ross and Watkins, \{W. M.\} and Sibley, \{C. H.\}",

note = "Funding Information: We thank the director of Kenya Medical Research Institute for permission to publish these data. This work was supported by the Wellcome Trust of Great Britain (grant ref. Nos. 045010 and 056769), the UNDP/World Bank/WHO Special program for Research and Training in Tropical Diseases (980369) and NIH grant AI 42321 to CHS. A.M.N., E.K.M., E.N., A.R. and W.M.W. are grateful to the Wellcome Trust for personal support.",

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AU - Mberu, E. K.

AU - Nduati, E.

AU - Ross, A.

AU - Watkins, W. M.

AU - Sibley, C. H.

N1 - Funding Information: We thank the director of Kenya Medical Research Institute for permission to publish these data. This work was supported by the Wellcome Trust of Great Britain (grant ref. Nos. 045010 and 056769), the UNDP/World Bank/WHO Special program for Research and Training in Tropical Diseases (980369) and NIH grant AI 42321 to CHS. A.M.N., E.K.M., E.N., A.R. and W.M.W. are grateful to the Wellcome Trust for personal support.

PY - 2002/11

Y1 - 2002/11

N2 - The genotypes of merozoite surface protein-1, merozoite surface protein-2 and glutamine rich protein are frequently used to distinguish recrudescence from reinfection when parasitaemia reappears after antimalarial drug treatment. However, none of the previous reports has clearly assessed the change of genetic diversity following drug treatment. In the present study, we have assessed the impact of pyrimethamine/sulfadoxine and chlorproguanil/dapsone on the genetic diversity of isolates and the multiplicity of infection in patient isolates from Kilifi, Kenya. We have analysed the length polymorphism of merozoite surface protein-1, merozoite surface protein-2 and glutamine rich protein and the data clearly show that treatment with pyrimethamine/sulfadoxine and chlorproguanil/dapsone did not change the multiplicity of infection found in patients, in contrast to the selection that these drugs exert on the genes encoded by the target enzymes. In addition, we report that children of less than 2 years tend to have fewer numbers of clones per isolate when compared with older children. Overall, this study shows that the selection for genes that confer drug resistance is not a factor in reducing the genetic diversity of parasite clones in a patient.

AB - The genotypes of merozoite surface protein-1, merozoite surface protein-2 and glutamine rich protein are frequently used to distinguish recrudescence from reinfection when parasitaemia reappears after antimalarial drug treatment. However, none of the previous reports has clearly assessed the change of genetic diversity following drug treatment. In the present study, we have assessed the impact of pyrimethamine/sulfadoxine and chlorproguanil/dapsone on the genetic diversity of isolates and the multiplicity of infection in patient isolates from Kilifi, Kenya. We have analysed the length polymorphism of merozoite surface protein-1, merozoite surface protein-2 and glutamine rich protein and the data clearly show that treatment with pyrimethamine/sulfadoxine and chlorproguanil/dapsone did not change the multiplicity of infection found in patients, in contrast to the selection that these drugs exert on the genes encoded by the target enzymes. In addition, we report that children of less than 2 years tend to have fewer numbers of clones per isolate when compared with older children. Overall, this study shows that the selection for genes that confer drug resistance is not a factor in reducing the genetic diversity of parasite clones in a patient.

KW - Antifolates

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ER -

Genetic diversity of Plasmodium falciparum parasites from Kenya is not affected by antifolate drug selection

Abstract

Bibliographical note

Keywords

ASJC Scopus subject areas

UN SDGs

Access to Document

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