Genetic architecture of gene expression in ovine skeletal muscle

L.J.A. Kogelman; K. Byrne; T. Vuocolo; N.S. Watson-Haigh; H.N. Kadarmideen; J.W. Kijas; H.V. Oddy; G.E. Gardner; C. Gondro; R.L. Tellam

doi:10.1186/1471-2164-12-607

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Genetic architecture of gene expression in ovine skeletal muscle

Journal article

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Peer reviewed

Genetic architecture of gene expression in ovine skeletal muscle

L.J.A. Kogelman, K. Byrne, T. Vuocolo, N.S. Watson-Haigh, H.N. Kadarmideen, J.W. Kijas, H.V. Oddy, G.E. Gardner, C. Gondro and R.L. Tellam

BMC Genomics, Vol.12, Article number: 607

2011

DOI: https://doi.org/10.1186/1471-2164-12-607

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Abstract

In livestock populations the genetic contribution to muscling is intensively monitored in the progeny of industry sires and used as a tool in selective breeding programs. The genes and pathways conferring this genetic merit are largely undefined. Genetic variation within a population has potential, amongst other mechanisms, to alter gene expression via cis- or trans-acting mechanisms in a manner that impacts the functional activities of specific pathways that contribute to muscling traits. By integrating sire-based genetic merit information for a muscling trait with progeny-based gene expression data we directly tested the hypothesis that there is genetic structure in the gene expression program in ovine skeletal muscle. Results The genetic performance of six sires for a well defined muscling trait, longissimus lumborum muscle depth, was measured using extensive progeny testing and expressed as an Estimated Breeding Value by comparison with contemporary sires. Microarray gene expression data were obtained for longissimus lumborum samples taken from forty progeny of the six sires (4-8 progeny/sire). Initial unsupervised hierarchical clustering analysis revealed strong genetic architecture to the gene expression data, which also discriminated the sire-based Estimated Breeding Value for the trait. An integrated systems biology approach was then used to identify the major functional pathways contributing to the genetics of enhanced muscling by using both Estimated Breeding Value weighted gene co-expression network analysis and a differential gene co-expression network analysis. The modules of genes revealed by these analyses were enriched for a number of functional terms summarised as muscle sarcomere organisation and development, protein catabolism (proteosome), RNA processing, mitochondrial function and transcriptional regulation. Conclusions This study has revealed strong genetic structure in the gene expression program within ovine longissimus lumborum muscle. The balance between muscle protein synthesis, at the levels of both transcription and translation control, and protein catabolism mediated by regulated proteolysis is likely to be the primary determinant of the genetic merit for the muscling trait in this sheep population. There is also evidence that high genetic merit for muscling is associated with a fibre type shift toward fast glycolytic fibres. This study provides insight into mechanisms, presumably subject to strong artificial selection, that underpin enhanced muscling in sheep populations.

Details

Title: Genetic architecture of gene expression in ovine skeletal muscle
Authors/Creators: L.J.A. Kogelman (Author/Creator)
K. Byrne (Author/Creator)
T. Vuocolo (Author/Creator)
N.S. Watson-Haigh (Author/Creator)
H.N. Kadarmideen (Author/Creator)
J.W. Kijas (Author/Creator)
H.V. Oddy (Author/Creator)
G.E. Gardner (Author/Creator)
C. Gondro (Author/Creator)
R.L. Tellam (Author/Creator)
Publication Details: BMC Genomics, Vol.12, Article number: 607
Publisher: BioMed Central
Identifiers: 991005542070107891
Copyright: © 2011 Kogelman et al
Murdoch Affiliation: School of Veterinary and Biomedical Sciences
Language: English
Resource Type: Journal article
Note: This is an Open Access article distributed under the terms of the Creative Commons Attribution License (http://creativecommons.org/licenses/by/2.0), which permits unrestricted use, distribution, and reproduction in any medium, provided the original work is properly cited.

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Collaboration types: Domestic collaboration; International collaboration
Citation topics: 1 Clinical & Life Sciences; 1.54 Molecular & Cell Biology - Genetics; 1.54.79 Genomic Bioinformatics
Web Of Science research areas: Biotechnology & Applied Microbiology; Genetics & Heredity
ESI research areas: Molecular Biology & Genetics