Analysis of copy number variations among diverse cattle breeds

Author:

Liu George E.,Hou Yali,Zhu Bin,Cardone Maria Francesca,Jiang Lu,Cellamare Angelo,Mitra Apratim,Alexander Leeson J.,Coutinho Luiz L.,Dell'Aquila Maria Elena,Gasbarre Lou C.,Lacalandra Gianni,Li Robert W.,Matukumalli Lakshmi K.,Nonneman Dan,Regitano Luciana C. de A.,Smith Tim P.L.,Song Jiuzhou,Sonstegard Tad S.,Van Tassell Curt P.,Ventura Mario,Eichler Evan E.,McDaneld Tara G.,Keele John W.

Abstract

Genomic structural variation is an important and abundant source of genetic and phenotypic variation. Here, we describe the first systematic and genome-wide analysis of copy number variations (CNVs) in modern domesticated cattle using array comparative genomic hybridization (array CGH), quantitative PCR (qPCR), and fluorescent in situ hybridization (FISH). The array CGH panel included 90 animals from 11 Bos taurus, three Bos indicus, and three composite breeds for beef, dairy, or dual purpose. We identified over 200 candidate CNV regions (CNVRs) in total and 177 within known chromosomes, which harbor or are adjacent to gains or losses. These 177 high-confidence CNVRs cover 28.1 megabases or ∼1.07% of the genome. Over 50% of the CNVRs (89/177) were found in multiple animals or breeds and analysis revealed breed-specific frequency differences and reflected aspects of the known ancestry of these cattle breeds. Selected CNVs were further validated by independent methods using qPCR and FISH. Approximately 67% of the CNVRs (119/177) completely or partially span cattle genes and 61% of the CNVRs (108/177) directly overlap with segmental duplications. The CNVRs span about 400 annotated cattle genes that are significantly enriched for specific biological functions, such as immunity, lactation, reproduction, and rumination. Multiple gene families, including ULBP, have gone through ruminant lineage-specific gene amplification. We detected and confirmed marked differences in their CNV frequencies across diverse breeds, indicating that some cattle CNVs are likely to arise independently in breeds and contribute to breed differences. Our results provide a valuable resource beyond microsatellites and single nucleotide polymorphisms to explore the full dimension of genetic variability for future cattle genomic research.

Publisher

Cold Spring Harbor Laboratory

Subject

Genetics(clinical),Genetics

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