The HLA‐B landscape of Africa: Signatures of pathogen‐driven selection and molecular identification of candidate alleles to malaria protection

Human leukocyte antigen (HLA) genes play a key role in the immune response to infectious diseases, some of which are highly prevalent in specific environments, like malaria in sub‐Saharan Africa. Former case–control studies showed that one particular HLA‐B allele, B*53, was associated with malaria p...

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Published inMolecular ecology Vol. 26; no. 22; pp. 6238 - 6252
Main Authors Sanchez‐Mazas, Alicia, Černý, Viktor, Di, Da, Buhler, Stéphane, Podgorná, Eliška, Chevallier, Elodie, Brunet, Lydie, Weber, Stephan, Kervaire, Barbara, Testi, Manuela, Andreani, Marco, Tiercy, Jean‐Marie, Villard, Jean, Nunes, José Manuel
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LanguageEnglish
Published England Blackwell Publishing Ltd 01.11.2017
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Abstract Human leukocyte antigen (HLA) genes play a key role in the immune response to infectious diseases, some of which are highly prevalent in specific environments, like malaria in sub‐Saharan Africa. Former case–control studies showed that one particular HLA‐B allele, B*53, was associated with malaria protection in Gambia, but this hypothesis was not tested so far within a population genetics framework. In this study, our objective was to assess whether pathogen‐driven selection associated with malaria contributed to shape the HLA‐B genetic landscape of Africa. To that aim, we first typed the HLA‐A and ‐B loci in 484 individuals from 11 populations living in different environments across the Sahel, and we analysed these data together with those available for 29 other populations using several approaches including linear modelling on various genetic, geographic and environmental parameters. In addition to relevant signatures of populations’ demography and migrations history in the genetic differentiation patterns of both HLA‐A and ‐B loci, we found that the frequencies of three HLA alleles, B*53, B*78 and A*74, were significantly associated with Plasmodium falciparum malaria prevalence, suggesting their increase through pathogen‐driven selection in malaria‐endemic environments. The two HLA‐B alleles were further identified, by high‐throughput sequencing, as B*53:01:01 (in putative linkage disequilibrium with one HLA‐C allele, C*04:01:01:01) and B*78:01 in all but one individuals tested, making them appropriate candidates to malaria protection. These results highlight the role of environmental factors in the evolution of the HLA polymorphism and open key perspectives for functional studies focusing on HLA peptide‐binding properties.
AbstractList Abstract Human leukocyte antigen ( HLA ) genes play a key role in the immune response to infectious diseases, some of which are highly prevalent in specific environments, like malaria in sub‐Saharan Africa. Former case–control studies showed that one particular HLA ‐B allele, B*53, was associated with malaria protection in Gambia, but this hypothesis was not tested so far within a population genetics framework. In this study, our objective was to assess whether pathogen‐driven selection associated with malaria contributed to shape the HLA ‐B genetic landscape of Africa. To that aim, we first typed the HLA ‐A and ‐B loci in 484 individuals from 11 populations living in different environments across the Sahel, and we analysed these data together with those available for 29 other populations using several approaches including linear modelling on various genetic, geographic and environmental parameters. In addition to relevant signatures of populations’ demography and migrations history in the genetic differentiation patterns of both HLA ‐A and ‐B loci, we found that the frequencies of three HLA alleles, B*53, B*78 and A*74, were significantly associated with Plasmodium falciparum malaria prevalence, suggesting their increase through pathogen‐driven selection in malaria‐endemic environments. The two HLA ‐B alleles were further identified, by high‐throughput sequencing, as B*53:01:01 (in putative linkage disequilibrium with one HLA ‐C allele, C*04:01:01:01) and B*78:01 in all but one individuals tested, making them appropriate candidates to malaria protection. These results highlight the role of environmental factors in the evolution of the HLA polymorphism and open key perspectives for functional studies focusing on HLA peptide‐binding properties.
Human leukocyte antigen (HLA) genes play a key role in the immune response to infectious diseases, some of which are highly prevalent in specific environments, like malaria in sub-Saharan Africa. Former case-control studies showed that one particular HLA-B allele, B*53, was associated with malaria protection in Gambia, but this hypothesis was not tested so far within a population genetics framework. In this study, our objective was to assess whether pathogen-driven selection associated with malaria contributed to shape the HLA-B genetic landscape of Africa. To that aim, we first typed the HLA-A and -B loci in 484 individuals from 11 populations living in different environments across the Sahel, and we analysed these data together with those available for 29 other populations using several approaches including linear modelling on various genetic, geographic and environmental parameters. In addition to relevant signatures of populations' demography and migrations history in the genetic differentiation patterns of both HLA-A and -B loci, we found that the frequencies of three HLA alleles, B*53, B*78 and A*74, were significantly associated with Plasmodium falciparum malaria prevalence, suggesting their increase through pathogen-driven selection in malaria-endemic environments. The two HLA-B alleles were further identified, by high-throughput sequencing, as B*53:01:01 (in putative linkage disequilibrium with one HLA-C allele, C*04:01:01:01) and B*78:01 in all but one individuals tested, making them appropriate candidates to malaria protection. These results highlight the role of environmental factors in the evolution of the HLA polymorphism and open key perspectives for functional studies focusing on HLA peptide-binding properties.
Author Podgorná, Eliška
Černý, Viktor
Kervaire, Barbara
Villard, Jean
Testi, Manuela
Weber, Stephan
Andreani, Marco
Di, Da
Brunet, Lydie
Chevallier, Elodie
Buhler, Stéphane
Nunes, José Manuel
Sanchez‐Mazas, Alicia
Tiercy, Jean‐Marie
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  surname: Nunes
  fullname: Nunes, José Manuel
  organization: Institute of Genetics and Genomics in Geneva (IGE3)
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Issue 22
Keywords pathogen-driven selection
malaria protection
geographic patterns
human population genetics
HLA polymorphism and disease associations
African populations
Language English
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2017 The Authors. Molecular Ecology Published by John Wiley & Sons Ltd.
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Snippet Human leukocyte antigen (HLA) genes play a key role in the immune response to infectious diseases, some of which are highly prevalent in specific environments,...
Abstract Human leukocyte antigen ( HLA ) genes play a key role in the immune response to infectious diseases, some of which are highly prevalent in specific...
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SubjectTerms Africa South of the Sahara
African populations
Alleles
Data processing
Demography
Disease Resistance - genetics
Environmental factors
Genetics
Genetics, Population
geographic patterns
Histocompatibility antigen HLA
HLA polymorphism and disease associations
HLA-B Antigens - genetics
human population genetics
Humans
Immune response
Immune system
Infectious diseases
Landscape
Leukocytes
Linkage Disequilibrium
Loci
Malaria
malaria protection
Malaria, Falciparum - genetics
Next-generation sequencing
Pathogens
pathogen‐driven selection
Plasmodium falciparum
Polymorphism
Population genetics
Populations
Signatures
Vector-borne diseases
Title The HLA‐B landscape of Africa: Signatures of pathogen‐driven selection and molecular identification of candidate alleles to malaria protection
URI https://onlinelibrary.wiley.com/doi/abs/10.1111%2Fmec.14366
https://www.ncbi.nlm.nih.gov/pubmed/28950417
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https://search.proquest.com/docview/1943648248
Volume 26
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