Hereditary β-mannosidosis in a dog: Clinicopathological and molecular genetic characterization

Pompei Bolfa; Ping Wang; Rajeev Nair; Sreekumari Rajeev; Anibal G Armien; Paula S Henthorn; Tim Wood; Mary Anna Thrall; Urs Giger

doi:10.1016/j.ymgme.2019.08.002

Hereditary β-mannosidosis in a dog: Clinicopathological and molecular genetic characterization

Mol Genet Metab. 2019 Sep-Oct;128(1-2):137-143. doi: 10.1016/j.ymgme.2019.08.002. Epub 2019 Aug 10.

Authors

Pompei Bolfa¹, Ping Wang², Rajeev Nair³, Sreekumari Rajeev⁴, Anibal G Armien⁵, Paula S Henthorn², Tim Wood⁶, Mary Anna Thrall⁴, Urs Giger²

Affiliations

¹ Department of Biomedical Sciences, Ross University School of Veterinary Medicine, PO Box 334, Basseterre, Saint Kitts and Nevis. Electronic address: pompeibolfa@gmail.com.
² Section of Medical Genetics (PennGen), School of Veterinary Medicine, University of Pennsylvania, 3900 Delancey St., Philadelphia, PA 19104-6010, USA.
³ Department of Clinical Sciences, Ross University School of Veterinary Medicine, PO Box 334, Basseterre, Saint Kitts and Nevis.
⁴ Department of Biomedical Sciences, Ross University School of Veterinary Medicine, PO Box 334, Basseterre, Saint Kitts and Nevis.
⁵ Ultrastructural Pathology Unit, Veterinary Diagnostic Laboratory, University of Minnesota, 1333 Gortner Avenue, St. Paul, MN 55108, USA.
⁶ Biochemical Genetics Laboratory, Greenwood Genetic Center, 106 Gregor Mendel Circle, Greenwood, SC 29646, USA.

Abstract

Hereditary β-mannosidosis causing progressive lysosomal neuropathy and other clinical signs, has been previously described in humans, Nubian goats, and Salers cattle. Here we report the clinicopathological, metabolic, and molecular genetic features of canine beta-mannosidase (MANBA, EC 3.2.1.25) deficiency. A 1-year-old male mix-breed dog from St. Kitts was presented with progressive stumbling, weakness, and regurgitation. Vacuolated lymphocytes were observed on the blood film. Postmortem findings included marked enlargement of nerves, megaesophagus, and internal hydrocephalus. Vacuolated macrophages, neurons, and secretory epithelial cells suggested an oligosaccharide storage disease. Plasma concentration of the β-mannosidosis specific oligosaccharide was approximately 75 fold that of controls. The plasma beta-mannosidase activity was severely reduced to ~5% of controls; five other lysosomal acid hydrolase activities were increased or within their normal reference interval. Genomic sequencing of this dog's MANBA gene identified a homozygous exonic five bp tandem duplication in the penultimate exon of the MANBA gene (c.2377_2381dupTATCA) which results in a reading frame shift, altering the subsequent amino acid sequence and creating a premature stop codon. The truncated beta-mannosidase enzyme is expected to be dysfunctional. This enzyme deficiency causes the accumulation of un-degraded oligosaccharides in cells, which affect the myelination of the peripheral and central nervous systems. This insertion was not encountered in 121 and 80-screened samples from dogs on St. Kitts (all were homozygous for wild-type) and Philadelphia region (wild-type), respectively. In conclusion, canine β-mannosidosis has similar clinicopathological features with some human patients, but milder signs than in ruminants and more severe than in knockout mice. Hence, dogs with β-mannosidosis could become a valuable disease model for the human disease.

Keywords: Animal model; Canine; Inborn error of metabolism; Lysosomal storage disease; MANBA gene; Mutation.

Publication types

Case Reports
Research Support, N.I.H., Extramural

MeSH terms

Animals
Codon, Nonsense
DNA Mutational Analysis
Dog Diseases / diagnosis
Dog Diseases / enzymology
Dog Diseases / genetics*
Dogs
Exons
Male
Mutation
beta-Mannosidase / genetics*
beta-Mannosidosis / diagnosis
beta-Mannosidosis / genetics*
beta-Mannosidosis / veterinary*

Substances

Codon, Nonsense
beta-Mannosidase

Grants and funding

P40 OD010939/OD/NIH HHS/United States