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Novel P397S MAPT variant associated with late onset and slow progressive frontotemporal dementia.


ABSTRACT: Mutations in the MAPT gene cause frontotemporal dementia with tau deposits. We report the novel p.P397S MAPT variant in eight subjects from five apparently nonrelated families suffering from frontotemporal dementia with autosomal dominant pattern of inheritance. In silico analysis reported conflicting evidence of pathogenicity. The segregation analysis support that this variant is likely pathogenic. The mean age at onset (61.4 years) and mean disease duration (13.9 years) of these subjects and their affected relatives were significantly higher compared with our series of p.P301L MAPT mutation carriers. These findings suggest that p.P397S variant could be a new MAPT mutation associated with a less aggressive phenotype than other MAPT mutations.

SUBMITTER: Borrego-Ecija S 

PROVIDER: S-EPMC6689677 | biostudies-literature | 2019 Aug

REPOSITORIES: biostudies-literature

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Novel P397S MAPT variant associated with late onset and slow progressive frontotemporal dementia.

Borrego-Écija Sergi S   Antonell Anna A   Puig-Butillé Joan Anton JA   Pericot Inmaculada I   Prat-Bravo Carme C   Abellan-Vidal Maria Teresa MT   Mallada Javier J   Olives Jaume J   Falgàs Neus N   Oliva Rafael R   Lladó Albert A   Sánchez-Valle Raquel R  

Annals of clinical and translational neurology 20190717 8


Mutations in the MAPT gene cause frontotemporal dementia with tau deposits. We report the novel p.P397S MAPT variant in eight subjects from five apparently nonrelated families suffering from frontotemporal dementia with autosomal dominant pattern of inheritance. In silico analysis reported conflicting evidence of pathogenicity. The segregation analysis support that this variant is likely pathogenic. The mean age at onset (61.4 years) and mean disease duration (13.9 years) of these subjects and t  ...[more]

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