Genotyping Assays for the Canine Degenerative Myelopathy-Associated c.118G&gt;A (p.E40K) Mutation of the &lt;i&gt;SOD1&lt;/i&gt; Gene Using Conventional and Real-Time PCR Methods: A High Prevalence in the Pembroke Welsh Corgi Breed in Japan

Chang, Hye-Sook; Kamishina, Hiroaki; Mizukami, Keijiro; Momoi, Yasuyuki; Katayama, Masaaki; Rahman, Mohammad Mahbubur; Uddin, Mohammad M.; Yabuki, Akira; Kohyama, Moeko; Yamato, Osamu

doi:10.1292/jvms.12-0451

Cited by 30 publications

(35 citation statements)

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“…The SOD1:c.118G > A mutation, associated with CDM, was originally identified in a genome-wide association study and characterised by sequence-based typing [ 13 ]. Recent studies have used conventional and real-time PCR techniques to develop more rapid and cost-effective methods of genotyping dogs for this particular mutation [ 14 – 16 ]. The present study employed PCR followed by RFLP analysis, utilising the Eco571 enzyme, demonstrating that this technique allows rapid and simple genotyping dogs for the SOD1:c.118G > A mutation.…”

Section: Discussionmentioning

confidence: 99%

A retrospective study of the prevalence of the canine degenerative myelopathy associated superoxide dismutase 1 mutation (SOD1:c.118G > A) in a referral population of German Shepherd dogs from the UK

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et al. 2014

Canine Genet Epidemiol

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BackgroundCanine degenerative myelopathy (CDM) is an adult onset, progressive neurodegenerative disease of the spinal cord. The disease was originally described in the German Shepherd dog (GSD), but it is now known to occur in many other dog breeds. A previous study has identified a mutation in the superoxide dismutase 1 gene (SOD1:c.118G > A) that is associated with susceptibility to CDM. In the present study, restriction fragment length polymorphism (RFLP) analysis was used to genotype GSD for SOD1:c.118G > A in order to estimate the prevalence of the mutation in a referral population of GSD in the UK.ResultsThis study demonstrated that the RFLP assay, based on use of PCR and subsequent digestion with the Eco571 enzyme, provided a simple genotyping test for the SOD1:c.118G > A mutation. In a young GSD population (i.e. dogs less than 6 years of age, before clinical signs of the disease usually become apparent), 8 of 50 dogs were found to be homozygous and a further 19 were heterozygous for the mutation. In dogs over 8 years of age, 21 of 50 dogs admitted to a tertiary referral hospital with pelvic limb ataxia as a major clinical sign were homozygous for the mutation, compared to none of 50 dogs of similar age, but where no neurological disease was reported on referral.ConclusionsThis data suggests that genotyping for the SOD1:c.118G > A mutation is clinically applicable and that the mutation has a high degree of penetrance. Genotyping might also be useful for screening the GSD population to avoid mating of two carriers, but since the allele frequency is relatively high in the UK population of GSD, care should be taken to avoid reduction in genetic diversity within the breed.

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Section: Discussionmentioning

confidence: 99%

A retrospective study of the prevalence of the canine degenerative myelopathy associated superoxide dismutase 1 mutation (SOD1:c.118G > A) in a referral population of German Shepherd dogs from the UK

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Price

Adams

et al. 2014

Canine Genet Epidemiol

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“…All dogs with A/A or A/G genotypes were PWC, while the three other dogs carrying G/G were two Beagles and a Maltese. The genotypes of the dogs used in the present study were determined using a previously reported real-time PCR method (Chang et al, 2013). Formalin-fixed paraffin-embedded sections of the caudal thoracic spinal cord were prepared from each dog.…”

Section: Immunohistochemistry Of Spinal Cordsmentioning

confidence: 99%

Accumulation and aggregate formation of mutant superoxide dismutase 1 in canine degenerative myelopathy

et al. 2015

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“…In a recent study (Chang et al, 2013), genotyping assays using conventional and real-time PCR methods were developed, and a preliminary genotyping survey was performed on 122 randomly selected PWCs without any CDM-related clinical signs, to determine the current allele frequency in Japan. Both of the assays provided clear-cut genotyping.…”

Section: Genetic and Molecular Findingsmentioning

confidence: 99%

Canine degenerative myelopathy: a model of human amyotrophic lateral sclerosis

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Höller

Taylor

et al. 2016

Zoology

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Genotyping Assays for the Canine Degenerative Myelopathy-Associated c.118G>A (p.E40K) Mutation of the <i>SOD1</i> Gene Using Conventional and Real-Time PCR Methods: A High Prevalence in the Pembroke Welsh Corgi Breed in Japan

Cited by 30 publications

References 12 publications

A retrospective study of the prevalence of the canine degenerative myelopathy associated superoxide dismutase 1 mutation (SOD1:c.118G > A) in a referral population of German Shepherd dogs from the UK

A retrospective study of the prevalence of the canine degenerative myelopathy associated superoxide dismutase 1 mutation (SOD1:c.118G > A) in a referral population of German Shepherd dogs from the UK

Accumulation and aggregate formation of mutant superoxide dismutase 1 in canine degenerative myelopathy

Canine degenerative myelopathy: a model of human amyotrophic lateral sclerosis

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