Novel COL5A1 variants and associated disease phenotypes in dogs with classical Ehlers‐Danlos syndrome

Author:

Bullock Garrett1,Jaffey Jared A.2ORCID,Cohn Leah A.3,Sox Erika4,Hostnik Eric T.5ORCID,Hutcheson Kyle D.6,Matero Erin7,Hoffmann Karen S.8,Johnson Gary S.1,Katz Martin L.9

Affiliation:

1. Department of Veterinary Pathobiology, College of Veterinary Medicine University of Missouri Columbia Missouri USA

2. Department of Specialty Medicine, College of Veterinary Medicine Midwestern University Glendale Arizona USA

3. Department of Veterinary Medicine and Surgery, Veterinary Health Center University of Missouri Columbia Missouri USA

4. Department of Small Animal Internal Medicine Ethos Veterinary Emergency and Referral Center Honolulu Hawaii USA

5. Department of Veterinary Clinical Sciences, Veterinary Medical Center Ohio State University Columbus Ohio USA

6. Saguaro Veterinary Surgery Tucson Arizona USA

7. Matero Veterinary Services Warren Michigan USA

8. Olney‐Sandy Spring Veterinary Hospital Sandy Spring Maryland USA

9. Mason Eye Institute University of Missouri Columbia Missouri USA

Abstract

AbstractBackgroundHuman patients with Ehlers‐Danlos syndrome (EDS) are categorized into subtypes based on causative genetic variants and phenotypes. The classical form of EDS, primarily caused by variants in COL5A1 or COL5A2, is a very common subtype in people but is poorly characterized in dogs.ObjectiveDescribe likely causal COL5A1 variants in dogs with classical EDS, summarize clinical histories, discuss potential disease mechanisms, and draw conclusions about disease prognosis.AnimalsSeven client‐owned dogs that exhibited clinical signs of classical EDS.MethodsClinical information was recorded from medical records and communication with attending veterinarians and dog owners. To identify potential causal gene sequence variants whole‐genome sequence analyses (n = 6) or Sanger sequencing (n = 1) were performed on DNA isolated from the probands. Pathological abnormalities in skin biopsy samples were assessed using histology and electron microscopy in 3 dogs.ResultsSix distinct heterozygous COL5A1 sequence variants were identified. The most common clinical signs included fragile skin (n = 7), hyperextensible skin (n = 7), joint hypermobility (n = 6), and atrophic scars (n = 5). The median age at last follow‐up or death was 12 years (range, 6.5‐14 years). Ultrastructural abnormalities in dermal collagen differed among dogs with different COL5A1 variants.Conclusion and Clinical ImportanceWe describe the genotypic and phenotypic spectrum of the classical subtype of EDS by identifying 6 novel COL5A1 variants in conjunction with detailed clinical histories that included long‐term follow‐up information in 7 dogs.

Publisher

Wiley

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