Molecular evolution of a malaria resistance gene (DARC) in primates
| Contribuinte(s) |
UNIVERSIDADE DE SÃO PAULO |
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| Data(s) |
30/10/2013
30/10/2013
2012
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| Resumo |
Genes involved in host-pathogen interactions are often strongly affected by positive natural selection. The Duffy antigen, coded by the Duffy antigen receptor for chemokines (DARC) gene, serves as a receptor for Plasmodium vivax in humans and for Plasmodium knowlesi in some nonhuman primates. In the majority of sub-Saharan Africans, a nucleic acid variant in GATA-1 of the gene promoter is responsible for the nonexpression of the Duffy antigen on red blood cells and consequently resistance to invasion by P. vivax. The Duffy antigen also acts as a receptor for chemokines and is expressed in red blood cells and many other tissues of the body. Because of this dual role, we sequenced a 3,000-bp region encompassing the entire DARC gene as well as part of its 5' and 3' flanking regions in a phylogenetic sample of primates and used statistical methods to evaluate the nature of selection pressures acting on the gene during its evolution. We analyzed both coding and regulatory regions of the DARC gene. The regulatory analysis showed accelerated rates of substitution at several sites near known motifs. Our tests of positive selection in the coding region using maximum likelihood by branch sites and maximum likelihood by codon sites did not yield statistically significant evidence for the action of positive selection. However, the maximum likelihood test in which the gene was subdivided into different structural regions showed that the known binding region for P. vivax/P. knowlesi is under very different selective pressures than the remainder of the gene. In fact, most of the gene appears to be under strong purifying selection, but this is not evident in the binding region. We suggest that the binding region is under the influence of two opposing selective pressures, positive selection possibly exerted by the parasite and purifying selection exerted by chemokines. PSC CUNY PSC CUNY C3IRG from City University of New York C3IRG from City University of New York INCTC/CNPq INCTC/CNPq CTC/CEPID/FAPESP CTC/CEPID/FAPESP Regional Blood Center of Ribeirao Preto Regional Blood Center of Ribeirao Preto Millennium Institute/CNPq Millennium Institute/CNPq |
| Identificador |
IMMUNOGENETICS, NEW YORK, v. 64, n. 7, supl. 4, Part 1-2, pp. 497-505, JUL, 2012 0093-7711 http://www.producao.usp.br/handle/BDPI/36801 10.1007/s00251-012-0608-2 |
| Idioma(s) |
eng |
| Publicador |
SPRINGER NEW YORK |
| Relação |
IMMUNOGENETICS |
| Direitos |
closedAccess Copyright SPRINGER |
| Palavras-Chave | #POSITIVE SELECTION #DUFFY #COEVOLUTION #ANTIGEN #ERYTHROCYTE #PLASMODIUM VIVAX #DUFFY-BLOOD-GROUP #CODON-SUBSTITUTION MODELS #PLASMODIUM-VIVAX #ADAPTIVE EVOLUTION #NATURAL-SELECTION #LIGAND-BINDING #GROUP ANTIGEN #GROUP LOCUS #ANTIGEN/RECEPTOR #PARASITES #GENETICS & HEREDITY #IMMUNOLOGY |
| Tipo |
article original article publishedVersion |
