Cerebellar axonopathy in Shivers horses identified by spatial transcriptomic and proteomic analyses

Author:

Valberg Stephanie J.1ORCID,Williams Zoë J.2,Henry Marisa L.1,Finno Carrie J.3ORCID

Affiliation:

1. Department of Large Animal Clinical Sciences, College of Veterinary Medicine Michigan State University East Lansing Michigan USA

2. C. Wayne McIlwraith Translational Medicine, College of Veterinary Medicine and Biomedical Sciences Colorado State University Fort Collins Colorado USA

3. Department of Population Health and Reproduction, School of Veterinary Medicine University of California‐Davis Davis California USA

Abstract

AbstractBackgroundShivers in horses is characterized by abnormal hindlimb movement when walking backward and is proposed to be caused by a Purkinje cell (PC) axonopathy based on histopathology.ObjectivesDefine region‐specific differences in gene expression within the lateral cerebellar hemisphere and compare cerebellar protein expression between Shivers horses and controls.AnimalsCase‐control study of 5 Shivers and 4 control geldings ≥16.2 hands in height.MethodsUsing spatial transcriptomics, gene expression was compared between Shivers and control horses in PC soma and lateral cerebellar hemisphere white matter, consisting primarily of axons. Tandem‐mass‐tag (TMT‐11) proteomic analysis was performed on lateral cerebellar hemisphere homogenates.ResultsDifferences in gene expression between Shivers and control horses were evident in principal component analysis of axon‐containing white matter but not PC soma. In white matter, there were 455/1846 differentially expressed genes (DEG; 350 ↓DEG, 105 ↑DEG) between Shivers and controls, with significant gene set enrichment of the Toll‐Like Receptor 4 (TLR4) cascade, highlighting neuroinflammation. There were 50/936 differentially expressed proteins (DEP). The 27 ↓DEP highlighted loss of axonal proteins including intermediate filaments (5), myelin (3), cytoskeleton (2), neurite outgrowth (2), and Na/K ATPase (1). The 23 ↑DEP were involved in the extracellular matrix (7), cytoskeleton (7), redox balance (2), neurite outgrowth (1), signal transduction (1), and others.Conclusion and Clinical ImportanceOur findings support axonal degeneration as a characteristic feature of Shivers. Combined with histopathology, these findings are consistent with the known distinctive response of PC to injury where axonal changes occur without a substantial impact on PC soma.

Publisher

Wiley

Subject

General Veterinary

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