BMC Medical Genetics (Jun 2009)

Homozygosity and risk of childhood death due to invasive bacterial disease

  • Williams Thomas N,
  • Shafi Mohammed,
  • Mwangi Isaiah,
  • Berkley James A,
  • Amos William,
  • Lyons Emily J,
  • Newton Charles R,
  • Peshu Norbert,
  • Marsh Kevin,
  • Scott J Anthony G,
  • Hill Adrian VS

DOI
https://doi.org/10.1186/1471-2350-10-55
Journal volume & issue
Vol. 10, no. 1
p. 55

Abstract

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Abstract Background Genetic heterozygosity is increasingly being shown to be a key predictor of fitness in natural populations, both through inbreeding depression, inbred individuals having low heterozygosity, and also through chance linkage between a marker and a gene under balancing selection. One important component of fitness that is often highlighted is resistance to parasites and other pathogens. However, the significance of equivalent loci in human populations remains unclear. Consequently, we performed a case-control study of fatal invasive bacterial disease in Kenyan children using a genome-wide screen with microsatellite markers. Methods 148 cases, comprising children aged Results At five markers homozygosity was strongly associated with mortality (odds ratio range 4.7 – 12.2) with evidence of interactions between some markers. Mortality was associated with different non-overlapping marker groups in Gram positive and Gram negative bacterial disease. Homozygosity at susceptibility markers was common (prevalence 19–49%) and, with the large effect sizes, this suggests that bacterial disease mortality may be strongly genetically determined. Conclusion Balanced polymorphisms appear to be more widespread in humans than previously appreciated and play a critical role in modulating susceptibility to infectious disease. The effect sizes we report, coupled with the stochasticity of exposure to pathogens suggests that infection and mortality are far from random due to a strong genetic basis.