The prevalence of nine genetic disorders in a dog population from Belgium, the Netherlands and Germany.

The prevalence of nine genetic disorders in a dog population from Belgium, the Netherlands and Germany.

The objective of this study was to screen a dog population from Belgium, the Netherlands and Germany for the presence of mutant alleles associated with hip dysplasia (HD), degenerative myelopathy (DM), exercise-induced collapse (EIC), neuronal ceroid lipofuscinosis 4A (NCL), centronuclear myopathy (...

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Main Authors: Bart J G Broeckx, Frank Coopman, Geert E C Verhoeven, Wim Van Haeringen, Leanne van de Goor, Tim Bosmans, Ingrid Gielen, Jimmy H Saunders, Sandra S A Soetaert, Henri Van Bree, Christophe Van Neste, Filip Van Nieuwerburgh, Bernadette Van Ryssen, Elien Verelst, Katleen Van Steendam, Dieter Deforce
Format: Article
Language:English
Published: Public Library of Science (PLoS) 2013-01-01
Series:PLoS ONE
Online Access:https://www.ncbi.nlm.nih.gov/pmc/articles/pmid/24069350/pdf/?tool=EBI
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spelling doaj-cd806f54ba1a4a1a812d7d9467dee5822021-03-04T10:21:41ZengPublic Library of Science (PLoS)PLoS ONE1932-62032013-01-0189e7481110.1371/journal.pone.0074811The prevalence of nine genetic disorders in a dog population from Belgium, the Netherlands and Germany.Bart J G BroeckxFrank CoopmanGeert E C VerhoevenWim Van HaeringenLeanne van de GoorTim BosmansIngrid GielenJimmy H SaundersSandra S A SoetaertHenri Van BreeChristophe Van NesteFilip Van NieuwerburghBernadette Van RyssenElien VerelstKatleen Van SteendamDieter DeforceThe objective of this study was to screen a dog population from Belgium, the Netherlands and Germany for the presence of mutant alleles associated with hip dysplasia (HD), degenerative myelopathy (DM), exercise-induced collapse (EIC), neuronal ceroid lipofuscinosis 4A (NCL), centronuclear myopathy (HMLR), mucopolysaccharidosis VII (MPS VII), myotonia congenita (MG), gangliosidosis (GM1) and muscular dystrophy (Duchenne type) (GRMD). Blood samples (K3EDTA) were collected for genotyping with Kompetitive Allele Specific PCR (n = 476). Allele and genotype frequencies were calculated in those breeds with at least 12 samples (n = 8). Hardy-Weinberg equilibrium was tested. Genetic variation was identified for 4 out of 9 disorders: mutant alleles were found in 49, 15, 3 and 2 breeds for HD, DM, EIC and NCL respectively. Additionally, mutant alleles were identified in crossbreeds for both HD and EIC. For HD, DM, EIC and NCL mutant alleles were newly discovered in 43, 13, 2 and 1 breed(s), respectively. In 9, 2 and 1 breed(s) for DM, EIC and NCL respectively, the mutant allele was detected, but the respective disorder has not been reported in those breeds. For 5 disorders (HMLR, MPS VII, MG, GM1, GRMD), the mutant allele could not be identified in our population. For the other 4 disorders (HD, DM, EIC, NCL), prevalence of associated mutant alleles seems strongly breed dependent. Surprisingly, mutant alleles were found in many breeds where the disorder has not been reported to date.https://www.ncbi.nlm.nih.gov/pmc/articles/pmid/24069350/pdf/?tool=EBI
collection DOAJ
language English
format Article
sources DOAJ
author Bart J G Broeckx
Frank Coopman
Geert E C Verhoeven
Wim Van Haeringen
Leanne van de Goor
Tim Bosmans
Ingrid Gielen
Jimmy H Saunders
Sandra S A Soetaert
Henri Van Bree
Christophe Van Neste
Filip Van Nieuwerburgh
Bernadette Van Ryssen
Elien Verelst
Katleen Van Steendam
Dieter Deforce
spellingShingle Bart J G Broeckx
Frank Coopman
Geert E C Verhoeven
Wim Van Haeringen
Leanne van de Goor
Tim Bosmans
Ingrid Gielen
Jimmy H Saunders
Sandra S A Soetaert
Henri Van Bree
Christophe Van Neste
Filip Van Nieuwerburgh
Bernadette Van Ryssen
Elien Verelst
Katleen Van Steendam
Dieter Deforce
The prevalence of nine genetic disorders in a dog population from Belgium, the Netherlands and Germany.
PLoS ONE
author_facet Bart J G Broeckx
Frank Coopman
Geert E C Verhoeven
Wim Van Haeringen
Leanne van de Goor
Tim Bosmans
Ingrid Gielen
Jimmy H Saunders
Sandra S A Soetaert
Henri Van Bree
Christophe Van Neste
Filip Van Nieuwerburgh
Bernadette Van Ryssen
Elien Verelst
Katleen Van Steendam
Dieter Deforce
author_sort Bart J G Broeckx
title The prevalence of nine genetic disorders in a dog population from Belgium, the Netherlands and Germany.
title_short The prevalence of nine genetic disorders in a dog population from Belgium, the Netherlands and Germany.
title_full The prevalence of nine genetic disorders in a dog population from Belgium, the Netherlands and Germany.
title_fullStr The prevalence of nine genetic disorders in a dog population from Belgium, the Netherlands and Germany.
title_full_unstemmed The prevalence of nine genetic disorders in a dog population from Belgium, the Netherlands and Germany.
title_sort prevalence of nine genetic disorders in a dog population from belgium, the netherlands and germany.
publisher Public Library of Science (PLoS)
series PLoS ONE
issn 1932-6203
publishDate 2013-01-01
description The objective of this study was to screen a dog population from Belgium, the Netherlands and Germany for the presence of mutant alleles associated with hip dysplasia (HD), degenerative myelopathy (DM), exercise-induced collapse (EIC), neuronal ceroid lipofuscinosis 4A (NCL), centronuclear myopathy (HMLR), mucopolysaccharidosis VII (MPS VII), myotonia congenita (MG), gangliosidosis (GM1) and muscular dystrophy (Duchenne type) (GRMD). Blood samples (K3EDTA) were collected for genotyping with Kompetitive Allele Specific PCR (n = 476). Allele and genotype frequencies were calculated in those breeds with at least 12 samples (n = 8). Hardy-Weinberg equilibrium was tested. Genetic variation was identified for 4 out of 9 disorders: mutant alleles were found in 49, 15, 3 and 2 breeds for HD, DM, EIC and NCL respectively. Additionally, mutant alleles were identified in crossbreeds for both HD and EIC. For HD, DM, EIC and NCL mutant alleles were newly discovered in 43, 13, 2 and 1 breed(s), respectively. In 9, 2 and 1 breed(s) for DM, EIC and NCL respectively, the mutant allele was detected, but the respective disorder has not been reported in those breeds. For 5 disorders (HMLR, MPS VII, MG, GM1, GRMD), the mutant allele could not be identified in our population. For the other 4 disorders (HD, DM, EIC, NCL), prevalence of associated mutant alleles seems strongly breed dependent. Surprisingly, mutant alleles were found in many breeds where the disorder has not been reported to date.
url https://www.ncbi.nlm.nih.gov/pmc/articles/pmid/24069350/pdf/?tool=EBI
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