Canine RNF170 Single Base Deletion in a Naturally Occurring Model for Human Neuroaxonal Dystrophy.

Shawna R Cook Cleo Schwarz Julien Guevar Charles-Antoine Assenmacher Maeve Sheehy Nathan Fanzone Molly E Church Leonardo Murgiano Margret L Casal Vidhya Jagannathan Rodrigo Gutierrez-Quintana Mark Lowrie Frank Steffen Tosso Leeb Kari J Ekenstedt

Mov Disord

Department of Basic Medical Sciences, College of Veterinary Medicine, Purdue University, West Lafayette, Indiana, USA.

Published: November 2024

Neuroaxonal dystrophy (NAD) is an inherited neurodegenerative disorder characterized by swollen axons in the central nervous system, with a newly identified form affecting Miniature American Shepherds.
Clinical evaluations and genetic studies revealed that young adult dogs exhibited gait abnormalities, linked to a specific genetic mutation (a 1-bp deletion in the RNF170 gene) that follows an autosomal recessive inheritance pattern.
The findings suggest that this canine version of NAD shares similarities with human spastic paraplegia-85, making it a potential model for studying similar human conditions and testing therapies.

Background: Neuroaxonal dystrophy (NAD) is a group of inherited neurodegenerative disorders characterized primarily by the presence of spheroids (swollen axons) throughout the central nervous system. In humans, NAD is heterogeneous, both clinically and genetically. NAD has also been described to naturally occur in large animal models, such as dogs. A newly recognized disorder in Miniature American Shepherd dogs (MAS), consisting of a slowly progressive neurodegenerative syndrome, was diagnosed as NAD via histopathology.

Objectives: To describe the clinical and pathological phenotype together with the identification of the underlying genetic cause.

Methods: Clinical and postmortem evaluations, together with a genome-wide association study and autozygosity mapping approach, followed by whole-genome sequencing.

Results: Affected dogs were typically young adults and displayed an abnormal gait characterized by pelvic limb weakness and ataxia. The underlying genetic cause was identified as a 1-bp (base pair) deletion in RNF170 encoding ring finger protein 170, which perfectly segregates in an autosomal recessive pattern. This deletion is predicted to create a frameshift (XM_038559916.1:c.367delG) and early truncation of the RNF170 protein (XP_038415844.1:(p.Ala123Glnfs*11)). The age of this canine RNF170 variant was estimated at ~30 years, before the reproductive isolation of the MAS breed.

Conclusions: RNF170 variants were previously identified in human patients with autosomal recessive spastic paraplegia-85 (SPG85); this clinical phenotype shows similarities to the dogs described herein. We therefore propose that this novel MAS NAD could serve as an excellent large animal model for equivalent human diseases, particularly since affected dogs demonstrate a relatively long lifespan, which represents an opportunity for therapeutic trials. © 2024 The Author(s). Movement Disorders published by Wiley Periodicals LLC on behalf of International Parkinson and Movement Disorder Society.

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