Genomic Prediction of Autotetraploids; Influence of Relationship Matrices, Allele Dosage, and Continuous Genotyping Calls in Phenotype Prediction

Author:

de Bem Oliveira Ivone12,Resende Marcio F R3,Ferrão Luis Felipe V1,Amadeu Rodrigo R1,Endelman Jeffrey B4,Kirst Matias5,Coelho Alexandre S G2,Munoz Patricio R1

Affiliation:

1. Blueberry Breeding and Genomics Lab

2. Plant Genetics and Genomics Lab, Agronomy College, Federal University of Goias, GO, Brazil, 74690-900

3. Sweet Corn Genomics and Breeding, Horticultural Sciences Department, University of Florida, Gainesville, FL 32611

4. Department of Horticulture, University of Wisconsin, Madison, WI 53706

5. Forest Genomics Lab, School of Forestry Resources and Conservation, University of Florida, Gainesville, FL 32610

Abstract

Abstract Estimation of allele dosage, using genomic data, in autopolyploids is challenging and current methods often result in the misclassification of genotypes. Some progress has been made when using SNP arrays, but the major challenge is when using next generation sequencing data. Here we compare the use of read depth as continuous parameterization with ploidy parameterizations in the context of genomic selection (GS). Additionally, different sources of information to build relationship matrices were compared. A real breeding population of the autotetraploid species blueberry (Vaccinium corybosum), composed of 1,847 individuals was phenotyped for eight yield and fruit quality traits over two years. Continuous genotypic based models performed as well as the best models. This approach also reduces the computational time and avoids problems associated with misclassification of genotypic classes when assigning dosage in polyploid species. This approach could be very valuable for species with higher ploidy levels or for emerging crops where ploidy is not well understood. To our knowledge, this work constitutes the first study of genomic selection in blueberry. Accuracies are encouraging for application of GS for blueberry breeding. GS could reduce the time for cultivar release by three years, increasing the genetic gain per cycle by 86% on average when compared to phenotypic selection, and 32% when compared with pedigree-based selection. Finally, the genotypic and phenotypic data used in this study are made available for comparative analysis of dosage calling and genomic selection prediction models in the context of autopolyploids.

Publisher

Oxford University Press (OUP)

Subject

Genetics(clinical),Genetics,Molecular Biology

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