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Genome-wide association and systems genetic analyses of residual feed intake, daily feed consumption, backfat and weight gain in pigs
- Source :
- BMC Genetics, Ngoc Do, D, Ostersen, T, Strathe, A B, Mark, T, Jensen, J & Kadarmideen, H N 2014, ' Genome-wide association and systems genetic analyses of residual feed intake, daily feed consumption, backfat and weight gain in pigs ', B M C Genetics, vol. 15, 27 . https://doi.org/10.1186/1471-2156-15-27, Do, D N, Ostersen, T, Mark, T, Jensen, J & Kadarmideen, H 2014, ' Genome-wide association and systems genetic analyses of residual feed intake, daily feed consumtion, backfat and weight gain in pigs ' BMC genetics, vol 15, no. 27 ., 10.1186/1471-2156-15-27
- Publication Year :
- 2013
-
Abstract
- BackgroundFeed efficiency is one of the major components determining costs of animal production. Residual feed intake (RFI) is defined as the difference between the observed and the expected feed intake given a certain production. Residual feed intake 1 (RFI1) was calculated based on regression of individual daily feed intake (DFI) on initial test weight and average daily gain. Residual feed intake 2 (RFI2) was as RFI1 except it was also regressed with respect to backfat (BF). It has been shown to be a sensitive and accurate measure for feed efficiency in livestock but knowledge of the genomic regions and mechanisms affecting RFI in pigs is lacking. The study aimed to identify genetic markers and candidate genes for RFI and its component traits as well as pathways associated with RFI in Danish Duroc boars by genome-wide associations and systems genetic analyses.ResultsPhenotypic and genotypic records (using the Illumina Porcine SNP60 BeadChip) were available on 1,272 boars. Fifteen and 12 loci were significantly associated (p < 1.52 x 10-6) with RFI1 and RFI2, respectively. Among them, 10 SNPs were significantly associated with both RFI1 and RFI2 implying the existence of common mechanisms controlling the two RFI measures. Significant QTL regions for component traits of RFI (DFI and BF) were detected on pig chromosome (SSC) 1 (for DFI) and 2 for (BF). The SNPs within MAP3K5 and PEX7 on SSC 1, ENSSSCG00000022338 on SSC 9, and DSCAM on SSC 13 might be interesting markers for both RFI measures. Functional annotation of genes in 0.5 Mb size flanking significant SNPs indicated regulation of protein and lipid metabolic process, gap junction, inositol phosphate metabolism and insulin signaling pathway are significant biological processes and pathways for RFI, respectively.ConclusionsThe study detected novel genetic variants and QTLs on SSC 1, 8, 9, 13 and 18 for RFI and indicated significant biological processes and metabolic pathways involved in RFI. The study also detected novel QTLs for component traits of RFI. These results improve our knowledge of the genetic architecture and potential biological pathways underlying RFI; which would be useful for further investigations of key candidate genes for RFI and for development of biomarkers.
- Subjects :
- Male
Candidate gene
Sus scrofa
Genome-wide association study
Weight Gain
Linkage Disequilibrium
CANDIDATE GENES
Eating
Body Fat Distribution
GWAS
Genetics(clinical)
Genetics (clinical)
Systems genetics
2. Zero hunger
Genetics
QUANTITATIVE TRAIT LOCI
0303 health sciences
Systems Biology
04 agricultural and veterinary sciences
Phenotype
BEEF-CATTLE
Pigs
Research Article
HAPLOTYPE BLOCKS
EFFICIENCY
Meat
Genotype
Animal feed
Quantitative Trait Loci
SIGNAL-TRANSDUCTION
Single-nucleotide polymorphism
Biology
Quantitative trait locus
Feed conversion ratio
Polymorphism, Single Nucleotide
03 medical and health sciences
Residual feed intake
Backfat
Animals
Pathways
POLYMORPHISMS
Genetic Association Studies
030304 developmental biology
RECEPTOR
0402 animal and dairy science
MEAT QUALITY TRAITS
040201 dairy & animal science
Animal Feed
Genetic architecture
GROWING PIGS
Haplotypes
Linear Models
Subjects
Details
- ISSN :
- 14712156
- Volume :
- 15
- Database :
- OpenAIRE
- Journal :
- BMC genetics
- Accession number :
- edsair.doi.dedup.....a18eba2cbf7358a4734f589343789427
- Full Text :
- https://doi.org/10.1186/1471-2156-15-27