Disruption of chromosome 11 in canine fibrosarcomas highlights an unusual variability of <it>CDKN2B </it>in dogs

Disruption of chromosome 11 in canine fibrosarcomas highlights an unusual variability of <it>CDKN2B </it>in dogs

<p>Abstract</p> <p>Background</p> <p>In dogs in the western world neoplasia constitutes the most frequently diagnosed cause of death. Although there appear to be similarities between canine and human cancers, rather little is known about the cytogenetic and molecular al...

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Main Authors: Haugland Sean, Hoather Tess, O'Brien Patricia CM, Queen Chris, Milne Bruce S, Aguirre-Hernández Jesús, Ferguson-Smith Malcolm A, Dobson Jane M, Sargan David R
Format: Article
Language:English
Published: BMC 2009-07-01
Series:BMC Veterinary Research
Online Access:http://www.biomedcentral.com/1746-6148/5/27
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spelling doaj-78db7b17d1324bcca5e31522d9468e932020-11-25T00:04:46ZengBMCBMC Veterinary Research1746-61482009-07-01512710.1186/1746-6148-5-27Disruption of chromosome 11 in canine fibrosarcomas highlights an unusual variability of <it>CDKN2B </it>in dogsHaugland SeanHoather TessO'Brien Patricia CMQueen ChrisMilne Bruce SAguirre-Hernández JesúsFerguson-Smith Malcolm ADobson Jane MSargan David R<p>Abstract</p> <p>Background</p> <p>In dogs in the western world neoplasia constitutes the most frequently diagnosed cause of death. Although there appear to be similarities between canine and human cancers, rather little is known about the cytogenetic and molecular alterations in canine tumours. Different dog breeds are susceptible to different types of cancer, but the genetic basis of the great majority of these predispositions has yet to be discovered. In some retriever breeds there is a high incidence of soft tissue sarcomas and we have previously reported alterations of chromosomes 11 and 30 in two poorly differentiated fibrosarcomas. Here we extend our observations and present a case report on detail rearrangements on chromosome 11 as well as genetic variations in a tumour suppressor gene in normal dogs.</p> <p>Results</p> <p>BAC hybridisations on metaphases of two fibrosarcomas showed complex rearrangements on chromosome 11, and loss of parts of this chromosome. Microsatellite markers on a paired tumour and blood DNA pointed to loss of heterozygosity on chromosome 11 in the <it>CDKN2B</it>-<it>CDKN2A </it>tumour suppressor gene cluster region. PCR and sequencing revealed the homozygous loss of coding sequences for these genes, except for exon 1β of <it>CDKN2A</it>, which codes for the N-terminus of p14<sup>ARF</sup>. For <it>CDKN2B </it>exon 1, two alleles were observed in DNA from blood; one of them identical to the sequence in the dog reference genome and containing 4 copies of a 12 bp repeat found only in the canine gene amongst all species so far sequenced; the other allele was shorter due to a missing copy of the repeat. Sequencing of this exon in 141 dogs from 18 different breeds revealed a polymorphic region involving a GGC triplet repeat and a GGGGACGGCGGC repeat. Seven alleles were recorded and sixteen of the eighteen breeds showed heterozygosity.</p> <p>Conclusion</p> <p>Complex chromosome rearrangements were observed on chromosome 11 in two Labrador retriever fibrosarcomas. The chromosome alterations were reflected in the loss of sequences corresponding to two tumour suppressor genes involved in cell-cycle progression. Sequencing of <it>CDKN2B </it>across many different breeds revealed a widespread polymorphism within the first exon of the gene, immediately before the ankyrin coding sequences.</p> http://www.biomedcentral.com/1746-6148/5/27
collection DOAJ
language English
format Article
sources DOAJ
author Haugland Sean
Hoather Tess
O'Brien Patricia CM
Queen Chris
Milne Bruce S
Aguirre-Hernández Jesús
Ferguson-Smith Malcolm A
Dobson Jane M
Sargan David R
spellingShingle Haugland Sean
Hoather Tess
O'Brien Patricia CM
Queen Chris
Milne Bruce S
Aguirre-Hernández Jesús
Ferguson-Smith Malcolm A
Dobson Jane M
Sargan David R
Disruption of chromosome 11 in canine fibrosarcomas highlights an unusual variability of <it>CDKN2B </it>in dogs
BMC Veterinary Research
author_facet Haugland Sean
Hoather Tess
O'Brien Patricia CM
Queen Chris
Milne Bruce S
Aguirre-Hernández Jesús
Ferguson-Smith Malcolm A
Dobson Jane M
Sargan David R
author_sort Haugland Sean
title Disruption of chromosome 11 in canine fibrosarcomas highlights an unusual variability of <it>CDKN2B </it>in dogs
title_short Disruption of chromosome 11 in canine fibrosarcomas highlights an unusual variability of <it>CDKN2B </it>in dogs
title_full Disruption of chromosome 11 in canine fibrosarcomas highlights an unusual variability of <it>CDKN2B </it>in dogs
title_fullStr Disruption of chromosome 11 in canine fibrosarcomas highlights an unusual variability of <it>CDKN2B </it>in dogs
title_full_unstemmed Disruption of chromosome 11 in canine fibrosarcomas highlights an unusual variability of <it>CDKN2B </it>in dogs
title_sort disruption of chromosome 11 in canine fibrosarcomas highlights an unusual variability of <it>cdkn2b </it>in dogs
publisher BMC
series BMC Veterinary Research
issn 1746-6148
publishDate 2009-07-01
description <p>Abstract</p> <p>Background</p> <p>In dogs in the western world neoplasia constitutes the most frequently diagnosed cause of death. Although there appear to be similarities between canine and human cancers, rather little is known about the cytogenetic and molecular alterations in canine tumours. Different dog breeds are susceptible to different types of cancer, but the genetic basis of the great majority of these predispositions has yet to be discovered. In some retriever breeds there is a high incidence of soft tissue sarcomas and we have previously reported alterations of chromosomes 11 and 30 in two poorly differentiated fibrosarcomas. Here we extend our observations and present a case report on detail rearrangements on chromosome 11 as well as genetic variations in a tumour suppressor gene in normal dogs.</p> <p>Results</p> <p>BAC hybridisations on metaphases of two fibrosarcomas showed complex rearrangements on chromosome 11, and loss of parts of this chromosome. Microsatellite markers on a paired tumour and blood DNA pointed to loss of heterozygosity on chromosome 11 in the <it>CDKN2B</it>-<it>CDKN2A </it>tumour suppressor gene cluster region. PCR and sequencing revealed the homozygous loss of coding sequences for these genes, except for exon 1β of <it>CDKN2A</it>, which codes for the N-terminus of p14<sup>ARF</sup>. For <it>CDKN2B </it>exon 1, two alleles were observed in DNA from blood; one of them identical to the sequence in the dog reference genome and containing 4 copies of a 12 bp repeat found only in the canine gene amongst all species so far sequenced; the other allele was shorter due to a missing copy of the repeat. Sequencing of this exon in 141 dogs from 18 different breeds revealed a polymorphic region involving a GGC triplet repeat and a GGGGACGGCGGC repeat. Seven alleles were recorded and sixteen of the eighteen breeds showed heterozygosity.</p> <p>Conclusion</p> <p>Complex chromosome rearrangements were observed on chromosome 11 in two Labrador retriever fibrosarcomas. The chromosome alterations were reflected in the loss of sequences corresponding to two tumour suppressor genes involved in cell-cycle progression. Sequencing of <it>CDKN2B </it>across many different breeds revealed a widespread polymorphism within the first exon of the gene, immediately before the ankyrin coding sequences.</p>
url http://www.biomedcentral.com/1746-6148/5/27
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