| Article ID | Journal | Published Year | Pages | File Type |
|---|---|---|---|---|
| 5629365 | Experimental Neurology | 2017 | 10 Pages |
â¢Striatal parvalbumin expression is decreased in the dystonic hamster model.â¢Density of Nkx2.1 labeled striatal interneurons was unchanged in dystonic hamsters.â¢BDNF and GABA-switch expression levels were not altered in dystonic hamsters.â¢GABAAR-α1 positive striatal neurons were transiently reduced in dystonic hamsters.â¢Retarded interneuron maturation could be involved in pathophysiology of dystonia.
GABAergic disinhibition has been suggested to play a critical role in the pathophysiology of several basal ganglia disorders, including dystonia, a common movement disorder. Previous studies have shown a deficit of striatal GABAergic interneurons (IN) in the dtsz mutant hamster, one of the few phenotypic animal models of dystonia. However, mechanisms underlying this deficit are largely unknown. In the present study, we investigated the migration and maturation of striatal IN during postnatal development (18Â days of age) and at age of highest severity of dystonia (33Â days of age) in this hamster model. In line with previous findings, the density of GAD67-positive IN and the level of parvalbumin mRNA, a marker for fast spiking GABAergic IN, were lower in the dtsz mutant than in control hamsters. However, an unaltered density of Nkx2.1 labeled cells and Nkx2.1 mRNA level suggested that the migration of GABAergic IN into the striatum was not retarded. Therefore, different factors that indicate maturation of GABAergic IN were determined. While mRNA of the KCC2 cation/chloride transporters and the cytosolic carboanhydrase VII, used as markers for the so called GABA switch, as well as BDNF were unaltered, we found a reduced number of IN expressing the alpha1 subunit of the GABAA-receptor (37.5%) in dtsz hamsters at an age of 33Â days, but not after spontaneous remission of dystonia at an age of 90Â days. Since IN shift expression from alpha2 to alpha1 subunits during postnatal maturation, this result together with a decreased parvalbumin mRNA expression suggest a delayed maturation of striatal GABAergic IN in this animal model, which might underlie abnormal neuronal activity and striatal plasticity.
