A New family with frontotemporal dementia with intronic 10+3 splice site mutation in the tau gene: neuropathology and molecular effects

Mutations in the tau gene cause familial frontotemporal dementia with parkinsonism linked to chromosome 17 characterized by filamentous tau protein deposits. Here we describe the clinical and neuropathological features of a case from a newly identified family with an intron 10+3‐splice site mutation in the tau gene. The proband presented with severe personality changes and stereotyped speech followed by parkinsonian symptoms. He died at age 56 after a disease duration of approximately 6 years. At autopsy, there was marked frontotemporal degeneration with abundant tau‐immunoreactive neuronal and glial inclusions widespread in the cortex and brainstem. RT‐PCR analysis revealed a 3.7‐fold increase of tau transcripts with exon 10, resulting in an 1.7‐fold higher expression level of 4‐repeat tau isoforms in soluble tau fractions when compared to control brains and exclusively 4‐repeat tau isoforms in the sarcosyl‐insoluble tau fractions. In accordance with the hypothesis that the overexpression leads to saturation of microtubule binding sites and an increase of unbound 4‐repeat tau isoforms which assemble into filaments, the neuronal and glial inclusions in this case were exclusively composed of 4‐repeat tau isoforms. The clinical and neuropathological data of this family are compared with  results  from  the  two  other  published  families  with the intron 10 + 3 mutation, the MSTD and the SOT 254 family.

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