HLA-DR3-DQ2 Mice Do Not Develop Ataxia in the Presence of High Titre Anti-gliadin Antibodies
- Author(s)
- Tarlac, V; Kelly, L; Nag, N; Allen-Graham, J; Anderson, RP; Storey, E;
- Details
- Publication Year 2013-06,Volume 12,Issue #3,Page 370-376
- Journal Title
- CEREBELLUM
- Publication Type
- Journal Article
- Abstract
- Recently, it has been suggested that anti-gliadin antibodies (alpha GAb) may produce "gluten ataxia", even in the absence of celiac disease enteropathy. alpha GAb are reportedly present in 12-50 % of patients with sporadic ataxia, but also in 12 % of the general population, such that the importance of alpha GAb as a cause of sporadic ataxia is not conclusively settled. We aimed to determine whether mice transgenic for HLA-DR3-DQ2 and immunised with gliadin to achieve high titres of alpha GAb would develop ataxia and/or cerebellar damage. From 6 weeks of age, HLA-DR3-DQ2 transgenic mice were immunised fortnightly with gliadin (n = 10) or a saline control (n = 6) in adjuvant. Serum titres were measured by alpha GAb enzyme-linked immunosorbent assay. At 24 weeks of age, mice were tested for locomotor function using the accelerating rotarod, ledged beam, ink-paw gait, and several neurological severity score subtests. Brains were then collected and processed for immunohistochemistry. Sections were analysed for lymphocytic infiltration, changes in morphology and Purkinje cell (PC) dendritic volume and the number of PCs counted via unbiased stereology. Gliadin-immunised mice developed high alpha GAb titres while controls did not. There was no statistically significant difference between the gliadin and sham-immunised HLA-DR3-DQ2 mice on any of the tests of motor coordination, in lymphocytic infiltration, PC number or in dendritic volume. High levels of alpha GAb are not sufficient to produce ataxia or cerebellar damage in HLA-DR3-DQ2 transgenic mice.
- Publisher
- SPRINGER
- Keywords
- IDIOPATHIC CEREBELLAR-ATAXIA; ADULT CELIAC-DISEASE; GLUTEN ATAXIA; TRANSGLUTAMINASE; SUSCEPTIBILITY; SENSITIVITY; INJURY; CELLS; MODEL
- Research Division(s)
- Immunology
- Publisher's Version
- https://doi.org/10.1007/s12311-012-0425-z
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Creation Date: 2013-06-01 12:00:00