Misidentification of runs of homozygosity islands in cattle caused by interference with copy number variation or large intermarker distances

Wilson Nandolo; Yuri T Utsunomiya; Gábor Mészáros; Maria Wurzinger; Negar Khayadzadeh; Rafaela B P Torrecilha; Henry A Mulindwa; Timothy N Gondwe; Patrik Waldmann; Maja Ferenčaković; José F Garcia; Benjamin D Rosen; Derek Bickhart; Curt P van Tassell; Ino Curik; Johann Sölkner

doi:10.1186/s12711-018-0414-x

Misidentification of runs of homozygosity islands in cattle caused by interference with copy number variation or large intermarker distances

Genet Sel Evol. 2018 Aug 22;50(1):43. doi: 10.1186/s12711-018-0414-x.

Authors

Wilson Nandolo^{1

2}, Yuri T Utsunomiya³, Gábor Mészáros⁴, Maria Wurzinger¹, Negar Khayadzadeh¹, Rafaela B P Torrecilha³, Henry A Mulindwa⁵, Timothy N Gondwe², Patrik Waldmann⁶, Maja Ferenčaković⁷, José F Garcia^{3

8}, Benjamin D Rosen⁹, Derek Bickhart⁹, Curt P van Tassell⁹, Ino Curik⁷, Johann Sölkner¹

Affiliations

¹ Division of Livestock Sciences (NUWI), University of Natural Resources and Life Sciences, Gregor-Mendel Strasse 33, 1180, Vienna, Austria.
² Lilongwe University of Agriculture and Natural Resources, P. O. Box 219, Lilongwe, Malawi.
³ School of Agricultural and Veterinarian Sciences, Jaboticabal, Department of Preventive Veterinary Medicine and Animal Reproduction, São Paulo State University (UNESP), São Paulo, Brazil.
⁴ Division of Livestock Sciences (NUWI), University of Natural Resources and Life Sciences, Gregor-Mendel Strasse 33, 1180, Vienna, Austria. gabor.meszaros@boku.ac.at.
⁵ National Livestock Resources Research Institute, P.O Box 96, Tororo, Uganda.
⁶ Department of Animal Breeding and Genetics, Swedish University of Agricultural Sciences, Box 7023, 750 07, Uppsala, Sweden.
⁷ Department of Animal Science, Faculty of Agriculture, University of Zagreb, Svetošimunska cesta 25, 10000, Zagreb, Croatia.
⁸ School of Veterinary Medicine, Araçatuba, Department of Support, Production and Animal Health, São Paulo State University (UNESP), São Paulo, Brazil.
⁹ Animal Genomics and Improvement Laboratory, Beltsville, MD, 20705-2350, USA.

Abstract

Background: Runs of homozygosity (ROH) islands are stretches of homozygous sequence in the genome of a large proportion of individuals in a population. Algorithms for the detection of ROH depend on the similarity of haplotypes. Coverage gaps and copy number variants (CNV) may result in incorrect identification of such similarity, leading to the detection of ROH islands where none exists. Misidentified hemizygous regions will also appear as homozygous based on sequence variation alone. Our aim was to identify ROH islands influenced by marker coverage gaps or CNV, using Illumina BovineHD BeadChip (777 K) single nucleotide polymorphism (SNP) data for Austrian Brown Swiss, Tyrol Grey and Pinzgauer cattle.

Methods: ROH were detected using clustering, and ROH islands were determined from population inbreeding levels for each marker. CNV were detected using a multivariate copy number analysis method and a hidden Markov model. SNP coverage gaps were defined as genomic regions with intermarker distances on average longer than 9.24 kb. ROH islands that overlapped CNV regions (CNVR) or SNP coverage gaps were considered as potential artefacts. Permutation tests were used to determine if overlaps between CNVR with copy losses and ROH islands were due to chance. Diversity of the haplotypes in the ROH islands was assessed by haplotype analyses.

Results: In Brown Swiss, Tyrol Grey and Pinzgauer, we identified 13, 22, and 24 ROH islands covering 26.6, 389.0 and 35.8 Mb, respectively, and we detected 30, 50 and 71 CNVR derived from CNV by using both algorithms, respectively. Overlaps between ROH islands, CNVR or coverage gaps occurred for 7, 14 and 16 ROH islands, respectively. About 37, 44 and 52% of the ROH islands coverage in Brown Swiss, Tyrol Grey and Pinzgauer, respectively, were affected by copy loss. Intersections between ROH islands and CNVR were small, but significantly larger compared to ROH islands at random locations across the genome, implying an association between ROH islands and CNVR. Haplotype diversity for reliable ROH islands was lower than for ROH islands that intersected with copy loss CNVR.

Conclusions: Our findings show that a significant proportion of the ROH islands in the bovine genome are artefacts due to CNV or SNP coverage gaps.

MeSH terms

Animals
Cattle / genetics*
DNA Copy Number Variations*
Genotyping Techniques / standards*
Haplotypes
Homozygote*
Polymorphism, Single Nucleotide

Grants and funding

HR 21/2016/OeAD-GmbH