Application of a Bayesian non-linear model hybrid scheme to sequence data for genomic prediction and QTL mapping

Tingting Wang; Yi-Ping Phoebe Chen; Iona M MacLeod; Jennie E Pryce; Michael E Goddard; Ben J Hayes

doi:10.1186/s12864-017-4030-x

Application of a Bayesian non-linear model hybrid scheme to sequence data for genomic prediction and QTL mapping

BMC Genomics. 2017 Aug 15;18(1):618. doi: 10.1186/s12864-017-4030-x.

Authors

Tingting Wang^{1

2

3}, Yi-Ping Phoebe Chen⁴, Iona M MacLeod^{5

6}, Jennie E Pryce^{5

6

7}, Michael E Goddard^{5

6

8}, Ben J Hayes^{5

6

9}

Affiliations

¹ School of Engineering and Mathematical Sciences, La Trobe University, Melbourne, VIC, 3083, Australia. tingting.wang@ecodev.vic.gov.au.
² Agriculture Victoria, AgriBio, Centre for AgriBioscience, Melbourne, VIC, 3083, Australia. tingting.wang@ecodev.vic.gov.au.
³ Dairy Futures Cooperative Research Centre, Melbourne, VIC, 3083, Australia. tingting.wang@ecodev.vic.gov.au.
⁴ School of Engineering and Mathematical Sciences, La Trobe University, Melbourne, VIC, 3083, Australia.
⁵ Agriculture Victoria, AgriBio, Centre for AgriBioscience, Melbourne, VIC, 3083, Australia.
⁶ Dairy Futures Cooperative Research Centre, Melbourne, VIC, 3083, Australia.
⁷ School of Applied Systems Biology, La Trobe University, Melbourne, VIC, 3083, Australia.
⁸ Faculty of Veterinary and Agricultural Science, University of Melbourne, Melbourne, VIC, 3010, Australia.
⁹ Queensland Alliance for Agriculture and Food Innovation, Centre for Animal Science, University of Queensland, St Lucia, Brisbane, QLD, 4072, Australia.

Abstract

Background: Using whole genome sequence data might improve genomic prediction accuracy, when compared with high-density SNP arrays, and could lead to identification of casual mutations affecting complex traits. For some traits, the most accurate genomic predictions are achieved with non-linear Bayesian methods. However, as the number of variants and the size of the reference population increase, the computational time required to implement these Bayesian methods (typically with Monte Carlo Markov Chain sampling) becomes unfeasibly long.

Results: Here, we applied a new method, HyB_BR (for Hybrid BayesR), which implements a mixture model of normal distributions and hybridizes an Expectation-Maximization (EM) algorithm followed by Markov Chain Monte Carlo (MCMC) sampling, to genomic prediction in a large dairy cattle population with imputed whole genome sequence data. The imputed whole genome sequence data included 994,019 variant genotypes of 16,214 Holstein and Jersey bulls and cows. Traits included fat yield, milk volume, protein kg, fat% and protein% in milk, as well as fertility and heat tolerance. HyB_BR achieved genomic prediction accuracies as high as the full MCMC implementation of BayesR, both for predicting a validation set of Holstein and Jersey bulls (multi-breed prediction) and a validation set of Australian Red bulls (across-breed prediction). HyB_BR had a ten fold reduction in compute time, compared with the MCMC implementation of BayesR (48 hours versus 594 hours). We also demonstrate that in many cases HyB_BR identified sequence variants with a high posterior probability of affecting the milk production or fertility traits that were similar to those identified in BayesR. For heat tolerance, both HyB_BR and BayesR found variants in or close to promising candidate genes associated with this trait and not detected by previous studies.

Conclusions: The results demonstrate that HyB_BR is a feasible method for simultaneous genomic prediction and QTL mapping with whole genome sequence in large reference populations.

MeSH terms

Algorithms
Animals
Bayes Theorem
Cattle
Chromosome Mapping*
Female
Fertility / genetics
Genomics*
Genotype
Markov Chains
Milk / metabolism
Monte Carlo Method
Nonlinear Dynamics*
Phenotype
Polymorphism, Single Nucleotide
Quantitative Trait Loci / genetics*
Whole Genome Sequencing*