Estimating genetic diversity across the neutral genome with the use of dense marker maps.docVIP
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Estimating genetic diversity across the neutral genome with the use of dense marker maps
Engelsma et al. Genetics Selection Evolution 2010, 42:12
/content/42/1/12
Genetics
Selection
Evolution
RESEARCH
Open Access
Estimating genetic diversity across the neutral Research
genome with the use of dense marker maps
Krista A Engelsma*1,2, Mario PL Calus1, Piter Bijma2 and Jack J Windig1,3
Abstract
Background: With the advent of high throughput DNA typing, dense marker maps have become available to
investigate genetic diversity on specific regions of the genome. The aim of this paper was to compare two marker
based estimates of the genetic diversity in specific genomic regions lying in between markers: IBD-based genetic
diversity and heterozygosity.
Methods: A computer simulated population was set up with individuals containing a single 1-Morgan chromosome
and 1665 SNP markers and from this one, an additional population was produced with a lower marker density i.e. 166
SNP markers. For each marker interval based on adjacent markers, the genetic diversity was estimated either by IBD
probabilities or heterozygosity. Estimates were compared to each other and to the true genetic diversity. The latter was
calculated for a marker in the middle of each marker interval that was not used to estimate genetic diversity.
Results: The simulated population had an average minor allele frequency of 0.28 and an LD (r2) of 0.26, comparable to
those of real livestock populations. Genetic diversities estimated by IBD probabilities and by heterozygosity were
positively correlated, and correlations with the true genetic diversity were quite similar for the simulated population
with a high marker density, both for specific regions (r = 0.19-0.20) and large regions (r = 0.61-0.64) over the genome.
For the population with a lower marker density, the correlation with the true genetic diversity turned out to be higher
for the IBD-based genetic diversity.
Conclusions: Genetic diversities of ungenotyped regions of the genome (i.e. between markers) estimated by IBD-
based met
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