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TECPR2 Associated Neuroaxonal Dystrophy in Spanish Water Dogs.

PloS one (2015-11-12)
Kerstin Hahn, Cecilia Rohdin, Vidhya Jagannathan, Peter Wohlsein, Wolfgang Baumgärtner, Frauke Seehusen, Ingo Spitzbarth, Rodrigo Grandon, Cord Drögemüller, Karin Hultin Jäderlund
ZUSAMMENFASSUNG

Clinical, pathological and genetic examination revealed an as yet uncharacterized juvenile-onset neuroaxonal dystrophy (NAD) in Spanish water dogs. Affected dogs presented with various neurological deficits including gait abnormalities and behavioral deficits. Histopathology demonstrated spheroid formation accentuated in the grey matter of the cerebral hemispheres, the cerebellum, the brain stem and in the sensory pathways of the spinal cord. Iron accumulation was absent. Ultrastructurally spheroids contained predominantly closely packed vesicles with a double-layered membrane, which were characterized as autophagosomes using immunohistochemistry. The family history of the four affected dogs suggested an autosomal recessive inheritance. SNP genotyping showed a single genomic region of extended homozygosity of 4.5 Mb in the four cases on CFA 8. Linkage analysis revealed a maximal parametric LOD score of 2.5 at this region. By whole genome re-sequencing of one affected dog, a perfectly associated, single, non-synonymous coding variant in the canine tectonin beta-propeller repeat-containing protein 2 (TECPR2) gene affecting a highly conserved region was detected (c.4009C>T or p.R1337W). This canine NAD form displays etiologic parallels to an inherited TECPR2 associated type of human hereditary spastic paraparesis (HSP). In contrast to the canine NAD, the spinal cord lesions in most types of human HSP involve the sensory and the motor pathways. Furthermore, the canine NAD form reveals similarities to cases of human NAD defined by widespread spheroid formation without iron accumulation in the basal ganglia. Thus TECPR2 should also be considered as candidate gene for human NAD. Immunohistochemistry and the ultrastructural findings further support the assumption, that TECPR2 regulates autophagosome accumulation in the autophagic pathways. Consequently, this report provides the first genetic characterization of juvenile canine NAD, describes the histopathological features associated with the TECPR2 mutation and provides evidence to emphasize the association between failure of autophagy and neurodegeneration.

MATERIALIEN
Produktnummer
Marke
Produktbeschreibung

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Formaldehyd -Lösung, ACS reagent, 37 wt. % in H2O, contains 10-15% Methanol as stabilizer (to prevent polymerization)
SAFC
Formaldehyd -Lösung, contains 10-15% methanol as stabilizer, 37 wt. % in H2O
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Glutaraldehyd -Lösung, Grade I, 25% in H2O, specially purified for use as an electron microscopy fixative
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Formaldehyd -Lösung, for molecular biology, BioReagent, ≥36.0% in H2O (T)
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Osmiumtetroxid -Lösung, 4 wt. % in H2O
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Glutaraldehyd -Lösung, Grade II, 25% in H2O
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Glutaraldehyd -Lösung, 50 wt. % in H2O
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Osmiumtetroxid, ReagentPlus®, 99.8%
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Osmiumtetroxid -Lösung, suitable for electron microscopy, 4% in H2O
Supelco
Formaldehyd -Lösung, stabilized with methanol, ~37 wt. % in H2O, certified reference material
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Osmiumtetroxid -Lösung, 2.5 wt. % in tert-butanol
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Glutaraldehyd -Lösung, Grade I, 50% in H2O, specially purified for use as an electron microscopy fixative or other sophisticated use
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Formaldehyd -Lösung, meets analytical specification of USP, ≥34.5 wt. %
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Glutaraldehyd -Lösung, Grade I, 70% in H2O, specially purified for use as an electron microscopy fixative or other sophisticated use
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Rabbit Serum, USDA approved, sterile-filtered, suitable for cell culture
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Osmiumtetroxid, ACS reagent, ≥98.0%
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Osmiumtetroxid -Lösung, suitable for electron microscopy, 2% in H2O
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Glutarsäure-Dialdehyd -Lösung, 50 wt. % in H2O, FCC