Dynamic nuclear envelope phenotype in rats overexpressing mutated human torsinA protein.

A three-base-pair deletion in the human gene is causative for the most common form of primary dystonia: the early-onset dystonia type 1 (DYT1 dystonia). The pathophysiological consequences of this mutation are still unknown. To study the pathology of the mutant torsinA (TOR1A) protein, we have generated a transgenic rat line that overexpresses the human mutant protein under the control of the human promoter.