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. 2016 May 27;7:96. doi: 10.3389/fgene.2016.00096

Table 4.

Predictive ability and bias of genomic breeding value (GEBV) for BCWD survival STATUS using four GS models with two genotyping platforms.

Genotyping platforma GS modelb Training samplec Validation sampled
Phenotyped Genotyped Effective SNPsf πg Fitted SNPsh hM2i Predictive abilityj Biask
Chip ssGBLUP 4492 652 40,710 Nal Na 0.45 0.46 0.24
Chip wssGBLUPe 4492 652 40,710 Na Na 0.45 0.43 0.14
Chip BayesB 583 583 40,744 0.995 204 0.44 0.26 0.14
Chip BayesC 583 583 40,744 0.995 204 0.44 0.31 0.15
RAD ssGBLUP 4492 649 10,052 Na Na 0.52 0.42 0.19
RAD wssGBLUP 4492 649 10,052 Na Na 0.52 0.40 0.13
RAD BayesB 579 579 10,059 0.980 201 0.43 0.40 0.23
RAD BayesC 579 579 10,059 0.980 201 0.54 0.35 0.14
a

The effective number of SNPs used was 40,710 and 10,052 from the Chip and RAD genotyping platforms, respectively.

b

Genomic selection models: single-step GBLUP (ssGBLUP); weighted ssGBLUP (wssGBLUP); Bayesian methods BayesB and BayesC; the GS analysis included only progeny of 2005 families.

c

The training sample included offspring from 10 full-sib 2005 families each with n = 38–80 offspring; BayesB and BayesC models included only fish that had both genotype and phenotype records (n = 579–583). In contrast, the ssGBLUP and wssGBLUP methods included also non-genotyped fish that had disease records (progeny of 2005 families).

d

The validation sample included 53 breeders (offspring of 2005 families that were included in training sample).

e

From wssGBLUP, iteration 2 results are presented; iteration 2 yielded higher accuracy GEBVs than iteration 3.

f

The analysis included SNPs and samples with a calling rate ≥0.70 and 0.90 for the RAD and Chip genotyping platforms, respectively.

g

Mixture parameter p specifies the proportion of loci with null effect.

h

Markers that are sampled as having non-zero effect (1−π) are fitted simultaneously in the multiple regression model.

i

Proportion of genetic variance explained by the markers (hM2).

j

The predictive ability (PA) was calculated using the mean progeny performance (MPP) of 31 progeny testing families that had as parents a pair of validation fish. The PA of GEBV was estimated as the correlation of mid-parent GEBV with MPP from each progeny testing family, PAGEBV = CORR(GEBV, MPP).

k

The bias of GEBV was defined as the regression coefficient of performance MPP on predicted mid-parent GEBV (βMPP.GEBV).

l

Na indicates either non-available or non-needed data cell.