Article

A 2cM genome-wide scan of European Holstein cattle affected by classical BSE

BMC Genetics 01/2010; DOI:http://www.doaj.org/doaj?func=openurl&genre=article&issn=14712156&date=2010&volume=11&issue=1&spage=20
Source: DOAJ

ABSTRACT Abstract

Background

Classical bovine spongiform encephalopathy (BSE) is an acquired prion disease that is invariably fatal in cattle and has been implicated as a significant human health risk. Polymorphisms that alter the prion protein of sheep or humans have been associated with variations in transmissible spongiform encephalopathy susceptibility or resistance. In contrast, there is no strong evidence that non-synonymous mutations in the bovine prion gene ( PRNP ) are associated with classical BSE disease susceptibility. However, two bovine PRNP insertion/deletion polymorphisms, one within the promoter region and the other in intron 1, have been associated with susceptibility to classical BSE. These associations do not explain the full extent of BSE susceptibility, and loci outside of PRNP appear to be associated with disease incidence in some cattle populations. To test for associations with BSE susceptibility, we conducted a genome wide scan using a panel of 3,072 single nucleotide polymorphism (SNP) markers on 814 animals representing cases and control Holstein cattle from the United Kingdom BSE epidemic.

Results

Two sets of BSE affected Holstein cattle were analyzed in this study, one set with known family relationships and the second set of paired cases with controls. The family set comprises half-sibling progeny from six sires. The progeny from four of these sires had previously been scanned with microsatellite markers. The results obtained from the current analysis of the family set yielded both some supporting and new results compared with those obtained in the earlier study. The results revealed 27 SNPs representing 18 chromosomes associated with incidence of BSE disease. These results confirm a region previously reported on chromosome 20, and identify additional regions on chromosomes 2, 14, 16, 21 and 28. This study did not identify a significant association near the PRNP in the family sample set. The only association found in the PRNP region was in the case-control sample set and this was not significant after multiple test correction. The genome scan of the case-control animals did not identify any associations that passed a stringent genome-wide significance threshold.

Conclusions

Several regions of the genome are statistically associated with the incidence of classical BSE in European Holstein cattle. Further investigation of loci on chromosomes 2, 14, 16, 20, 21 and 28 will be required to uncover any biological significance underlying these marker associations.

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Keywords

18 chromosomes
 
3,072 single nucleotide polymorphism
 
acquired prion disease
 
biological significance
 
bovine prion gene
 
bovine PRNP insertion/deletion polymorphisms
 
BSE disease
 
BSE susceptibility
 
classical BSE disease susceptibility
 
control Holstein cattle
 
disease incidence
 
European Holstein cattle
 
new results
 
non-synonymous mutations
 
prion protein
 
PRNP region
 
promoter region
 
significant human health risk
 
stringent genome-wide significance threshold
 
transmissible spongiform encephalopathy susceptibility