Positive selection of a CD36 nonsense variant in sub-Saharan Africa, but no association with severe malaria phenotypes

The prevalence of CD36 deficiency in East Asian and African populations suggests that the causal variants are under selection by severe malaria. Previous analysis of data from the International HapMap Project indicated that a CD36 haplotype bearing a nonsense mutation (T1264G; rs3211938) had undergo...

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Autores principales: Fry, Andrew E., Ghansa, Anita, Small, Kerrin S., Palma, Alejandro, Auburn, Sarah, Diakite, Mahamadou, Green, Angela, Campino, Susana, Teo, Yik Y., Clark, Taane G., Jeffreys, Anna E., Wilson, Jonathan, Jallow, Muminatou, Sisay-Joof, Fatou, Pinder, Margaret, Griffiths, Michael J., Peshu, Norbert, Williams, Thomas N., Newton, Charles R., Marsh, Kevin, Molyneux, Malcolm E., Taylor, Terrie E., Koram, Kwadwo A., Oduro, Abraham R., Rogers, William O., Rockett, Kirk A., Sabeti, Pardis C., Kwiatkowski, Dominic P.
Formato: Texto
Lenguaje:English
Publicado: Oxford University Press 2009
Materias:
Association Studies Articles
Acceso en línea:https://www.ncbi.nlm.nih.gov/pmc/articles/PMC2701331/
https://www.ncbi.nlm.nih.gov/pubmed/19403559
http://dx.doi.org/10.1093/hmg/ddp192
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author Fry, Andrew E.
Ghansa, Anita
Small, Kerrin S.
Palma, Alejandro
Auburn, Sarah
Diakite, Mahamadou
Green, Angela
Campino, Susana
Teo, Yik Y.
Clark, Taane G.
Jeffreys, Anna E.
Wilson, Jonathan
Jallow, Muminatou
Sisay-Joof, Fatou
Pinder, Margaret
Griffiths, Michael J.
Peshu, Norbert
Williams, Thomas N.
Newton, Charles R.
Marsh, Kevin
Molyneux, Malcolm E.
Taylor, Terrie E.
Koram, Kwadwo A.
Oduro, Abraham R.
Rogers, William O.
Rockett, Kirk A.
Sabeti, Pardis C.
Kwiatkowski, Dominic P.
author_facet Fry, Andrew E.
Ghansa, Anita
Small, Kerrin S.
Palma, Alejandro
Auburn, Sarah
Diakite, Mahamadou
Green, Angela
Campino, Susana
Teo, Yik Y.
Clark, Taane G.
Jeffreys, Anna E.
Wilson, Jonathan
Jallow, Muminatou
Sisay-Joof, Fatou
Pinder, Margaret
Griffiths, Michael J.
Peshu, Norbert
Williams, Thomas N.
Newton, Charles R.
Marsh, Kevin
Molyneux, Malcolm E.
Taylor, Terrie E.
Koram, Kwadwo A.
Oduro, Abraham R.
Rogers, William O.
Rockett, Kirk A.
Sabeti, Pardis C.
Kwiatkowski, Dominic P.
author_sort Fry, Andrew E.
collection PubMed
description The prevalence of CD36 deficiency in East Asian and African populations suggests that the causal variants are under selection by severe malaria. Previous analysis of data from the International HapMap Project indicated that a CD36 haplotype bearing a nonsense mutation (T1264G; rs3211938) had undergone recent positive selection in the Yoruba of Nigeria. To investigate the global distribution of this putative selection event, we genotyped T1264G in 3420 individuals from 66 populations. We confirmed the high frequency of 1264G in the Yoruba (26%). However, the 1264G allele is less common in other African populations and absent from all non-African populations without recent African admixture. Using long-range linkage disequilibrium, we studied two West African groups in depth. Evidence for recent positive selection at the locus was demonstrable in the Yoruba, although not in Gambians. We screened 70 variants from across CD36 for an association with severe malaria phenotypes, employing a case–control study of 1350 subjects and a family study of 1288 parent–offspring trios. No marker was significantly associated with severe malaria. We focused on T1264G, genotyping 10 922 samples from four African populations. The nonsense allele was not associated with severe malaria (pooled allelic odds ratio 1.0; 95% confidence interval 0.89–1.12; P = 0.98). These results suggest a range of possible explanations including the existence of alternative selection pressures on CD36, co-evolution between host and parasite or confounding caused by allelic heterogeneity of CD36 deficiency.
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spelling pubmed-27013312009-06-25 Positive selection of a CD36 nonsense variant in sub-Saharan Africa, but no association with severe malaria phenotypes Fry, Andrew E. Ghansa, Anita Small, Kerrin S. Palma, Alejandro Auburn, Sarah Diakite, Mahamadou Green, Angela Campino, Susana Teo, Yik Y. Clark, Taane G. Jeffreys, Anna E. Wilson, Jonathan Jallow, Muminatou Sisay-Joof, Fatou Pinder, Margaret Griffiths, Michael J. Peshu, Norbert Williams, Thomas N. Newton, Charles R. Marsh, Kevin Molyneux, Malcolm E. Taylor, Terrie E. Koram, Kwadwo A. Oduro, Abraham R. Rogers, William O. Rockett, Kirk A. Sabeti, Pardis C. Kwiatkowski, Dominic P. Hum Mol Genet Association Studies Articles The prevalence of CD36 deficiency in East Asian and African populations suggests that the causal variants are under selection by severe malaria. Previous analysis of data from the International HapMap Project indicated that a CD36 haplotype bearing a nonsense mutation (T1264G; rs3211938) had undergone recent positive selection in the Yoruba of Nigeria. To investigate the global distribution of this putative selection event, we genotyped T1264G in 3420 individuals from 66 populations. We confirmed the high frequency of 1264G in the Yoruba (26%). However, the 1264G allele is less common in other African populations and absent from all non-African populations without recent African admixture. Using long-range linkage disequilibrium, we studied two West African groups in depth. Evidence for recent positive selection at the locus was demonstrable in the Yoruba, although not in Gambians. We screened 70 variants from across CD36 for an association with severe malaria phenotypes, employing a case–control study of 1350 subjects and a family study of 1288 parent–offspring trios. No marker was significantly associated with severe malaria. We focused on T1264G, genotyping 10 922 samples from four African populations. The nonsense allele was not associated with severe malaria (pooled allelic odds ratio 1.0; 95% confidence interval 0.89–1.12; P = 0.98). These results suggest a range of possible explanations including the existence of alternative selection pressures on CD36, co-evolution between host and parasite or confounding caused by allelic heterogeneity of CD36 deficiency. Oxford University Press 2009-07-15 2009-04-29 /pmc/articles/PMC2701331/ /pubmed/19403559 http://dx.doi.org/10.1093/hmg/ddp192 Text en © 2009 The Author(s) http://creativecommons.org/licenses/by-nc/2.0/uk/ This is an Open Access article distributed under the terms of the Creative Commons Attribution Non-Commercial License (http://creativecommons.org/licenses/by-nc/2.0/uk/) which permits unrestricted non-commercial use, distribution, and reproduction in any medium, provided the original work is properly cited.
spellingShingle Association Studies Articles
Fry, Andrew E.
Ghansa, Anita
Small, Kerrin S.
Palma, Alejandro
Auburn, Sarah
Diakite, Mahamadou
Green, Angela
Campino, Susana
Teo, Yik Y.
Clark, Taane G.
Jeffreys, Anna E.
Wilson, Jonathan
Jallow, Muminatou
Sisay-Joof, Fatou
Pinder, Margaret
Griffiths, Michael J.
Peshu, Norbert
Williams, Thomas N.
Newton, Charles R.
Marsh, Kevin
Molyneux, Malcolm E.
Taylor, Terrie E.
Koram, Kwadwo A.
Oduro, Abraham R.
Rogers, William O.
Rockett, Kirk A.
Sabeti, Pardis C.
Kwiatkowski, Dominic P.
Positive selection of a CD36 nonsense variant in sub-Saharan Africa, but no association with severe malaria phenotypes
title Positive selection of a CD36 nonsense variant in sub-Saharan Africa, but no association with severe malaria phenotypes
title_full Positive selection of a CD36 nonsense variant in sub-Saharan Africa, but no association with severe malaria phenotypes
title_fullStr Positive selection of a CD36 nonsense variant in sub-Saharan Africa, but no association with severe malaria phenotypes
title_full_unstemmed Positive selection of a CD36 nonsense variant in sub-Saharan Africa, but no association with severe malaria phenotypes
title_short Positive selection of a CD36 nonsense variant in sub-Saharan Africa, but no association with severe malaria phenotypes
title_sort positive selection of a cd36 nonsense variant in sub-saharan africa, but no association with severe malaria phenotypes
topic Association Studies Articles
url https://www.ncbi.nlm.nih.gov/pmc/articles/PMC2701331/
https://www.ncbi.nlm.nih.gov/pubmed/19403559
http://dx.doi.org/10.1093/hmg/ddp192
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