Comparison of different genetic distances to test isolation by distance between populations

被引:0
|
作者
M Séré
S Thévenon
A M G Belem
T De Meeûs
机构
[1] CIRDES,
[2] UMR IRD/CIRAD 177,undefined
[3] Centre International de Recherche-Développement sur l’Elevage en zone Subhumide (CIRDES),undefined
[4] CIRAD,undefined
[5] UMR INTERTRYP,undefined
[6] IRD,undefined
[7] UMR Interactions Hôtes—Vecteurs—Parasites dans les Infections par des Trypanosomatidae—(INTERTRYP) IRD/CIRAD 177,undefined
[8] Université Polytechnique de Bobo-Dioulasso,undefined
来源
Heredity | 2017年 / 119卷
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摘要
Studying isolation by distance can provide useful demographic information. To analyze isolation by distance from molecular data, one can use some kind of genetic distance or coalescent simulations. Molecular markers can often display technical caveats, such as PCR-based amplification failures (null alleles, allelic dropouts). These problems can alter population parameter inferences that can be extracted from molecular data. In this simulation study, we analyze the behavior of different genetic distances in Island (null hypothesis) and stepping stone models displaying varying neighborhood sizes. Impact of null alleles of increasing frequency is also studied. In stepping stone models without null alleles, the best statistic to detect isolation by distance in most situations is the chord distance DCSE. Nevertheless, for markers with genetic diversities HS<0.4–0.5, all statistics tend to display the same statistical power. Marginal sub-populations behave as smaller neighborhoods. Metapopulations composed of small sub-population numbers thus display smaller neighborhood sizes. When null alleles are introduced, the power of detection of isolation by distance is significantly reduced and DCSE remains the most powerful genetic distance. We also show that the proportion of null allelic states interact with the slope of the regression of FST/(1−FST) as a function of geographic distance. This can have important consequences on inferences that can be made from such data. Nevertheless, Chapuis and Estoup’s FreeNA correction for null alleles provides very good results in most situations. We finally use our conclusions for reanalyzing and reinterpreting some published data sets.
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页码:55 / 63
页数:8
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