Scientific article
English

Distinct evolutionary strategies of human leucocyte antigen loci in pathogen-rich environments

Published inPhilosophical transactions - Royal Society. Biological sciences, vol. 367, no. 1590, p. 830-839
Publication date2012
Abstract

Human leucocyte antigen (HLA) loci have a complex evolution where both stochastic (e.g. genetic drift) and deterministic (natural selection) forces are involved. Owing to their extraordinary level of polymorphism, HLA genes are useful markers for reconstructing human settlement history. However, HLA variation often deviates significantly from neutral expectations towards an excess of genetic diversity. Because HLA molecules play a crucial role in immunity, this observation is generally explained by pathogen-driven-balancing selection (PDBS). In this study, we investigate the PDBS model by analysing HLA allelic diversity on a large database of 535 populations in relation to pathogen richness. Our results confirm that geographical distances are excellent predictors of HLA genetic differentiation worldwide. We also find a significant positive correlation between genetic diversity and pathogen richness at two HLA class I loci (HLA-A and -B), as predicted by PDBS, and a significant negative correlation at one HLA class II locus (HLA-DQB1). Although these effects are weak, as shown by a loss of significance when populations submitted to rapid genetic drift are removed from the analysis, the inverse relationship between genetic diversity and pathogen richness at different loci indicates that HLA genes have adopted distinct evolutionary strategies to provide immune protection in pathogen-rich environments.

Keywords
  • Human leucocyte antigen
  • Immunogenetics
  • Pathogen-driven-balancing selection
  • Pathogen richness
  • Human migrations
  • Genetic drift
Citation (ISO format)
SANCHEZ-MAZAS, Alicia, LEMAITRE, Jean-François, CURRAT, Mathias. Distinct evolutionary strategies of human leucocyte antigen loci in pathogen-rich environments. In: Philosophical transactions - Royal Society. Biological sciences, 2012, vol. 367, n° 1590, p. 830–839. doi: 10.1098/rstb.2011.0312
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Article (Published version)
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ISSN of the journal0962-8436
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