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Laboratory investigation; a journal of technical methods and pathology
Feb, 2011;91 (2): 216-31.

An intronic LINE-1 element insertion in the dystrophin gene aborts dystrophin expression and results in Duchenne-like muscular dystrophy in the corgi breed.

Bruce F Smith, Yongping Yue, Philip R Woods, Joe N Kornegay, Jin-Hong Shin, Regina R Williams, Dongsheng Duan
Author Information
  1. Bruce F Smith: Scott-Ritchey Research Center, College of Veterinary Medicine, Auburn University, Auburn, AL 36849, USA. smithbf@auburn.edu
PMID: 20714321 DOI: 10.1038/labinvest.2010.146

Abstract

Duchenne muscular dystrophy (DMD) is a dystrophin-deficient lethal muscle disease. To date, the catastrophic muscle wasting phenotype has only been seen in dystrophin-deficient humans and dogs. Although Duchenne-like symptoms have been observed in more than a dozen dog breeds, the mutation is often not known and research colonies are rarely established. Here, we report an independent canine DMD model originally derived from the Pembroke Welsh corgi breed. The affected dogs presented clinical signs of muscular dystrophy. Immunostaining revealed the absence of dystrophin and upregulation of utrophin. Histopathologic examination showed variable fiber size, central nucleation, calcification, fibrosis, neutrophil and macrophage infiltration and cardiac focal vacuolar degeneration. Carrier dogs also displayed mild myopathy. The mutation was identified as a long interspersed repetitive element-1 (LINE-1) insertion in intron 13, which introduced a new exon containing an in-frame stop codon. Similar mutations have been seen in human patients. A colony was generated by crossing carrier females with normal males. Affected puppies had a normal birth weight but they experienced a striking growth delay in the first 5 days. In summary, the new corgi DMD model offers an excellent opportunity to study DMD pathogenesis and to develop novel therapies.

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Grants

  1. AR-49419/NIAMS NIH HHS
  2. AR-48650/NIAMS NIH HHS
  3. AR-57209/NIAMS NIH HHS
  4. R01 AR049419/NIAMS NIH HHS
  5. R03 AR048650/NIAMS NIH HHS
  6. R21 AR057209-01A1/NIAMS NIH HHS
  7. R03 AR048650-03/NIAMS NIH HHS
  8. R01 AR049419-07/NIAMS NIH HHS
  9. R21 AR057209/NIAMS NIH HHS

MeSH Term

Analysis of Variance
Animals
Blotting, Western
Creatine Kinase
DNA Primers
Disease Models, Animal
Dogs
Dystrophin
Fluorescent Antibody Technique
Genotype
Histological Techniques
INDEL Mutation
Immunohistochemistry
Introns
Long Interspersed Nucleotide Elements
Muscle, Skeletal
Muscular Dystrophy, Duchenne
Utrophin

Chemicals

DNA Primers
Dystrophin
Utrophin
Creatine Kinase
Journal Article Research Support, N.I.H., Extramural Research Support, Non-U.S. Gov't

Word Cloud

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