Pattern of progression in MAPT‐related frontotemporal dementia: Results from the GENFI study

Emily Todd ,Adrian Danek,Alexander Gerhard,Martina Bocchetta,Harro Seelaar,Isabelle Le Ber,Mario Masellis,Markus Otto,Sandro Sorbi,Fabrizio Tagliavini,Johannes Levin,Elizabeth Finger,Lize C Jiskoot,Barbara Borroni,Maria Carmela Tartaglia,Georgia Peakman,Matthis Synofzik,Caroline Graff,Daniela Galimberti,Rik Vandenberghe,Simon Ducharme,Robert Laforce,Isabel Santana,Florence Pasquier,David M Cash ,Raquel Sánchez‐Valle ,David L Thomas ,Jonathan D Rohrer ,Alexandre De Mendonça ,John C Van Swieten ,James B Rowe ,Fermín Moreno ,Christopher R Butler ,Rhian S Convery ,Lucy L Russell ,Null Author_Id

doi:10.1002/alz.052265

Abstract

AbstractBackgroundMutations in MAPT are associated with frontotemporal dementia (FTD), but little is known about the progression in its early stages. We aimed at identifying the presence of early brain changes in MAPT mutation carriers.MethodWe included 3T MRIs from 84 MAPT carriers [27 symptomatic: mean(SD) age 58(8) years; 57 presymptomatic: 40(11) years] from the Genetic FTD Initiative (GENFI) and from 77 age‐matched non‐carrier healthy controls (44(14) years). Based on their expected years to symptom onset (EYO), we divided the presymptomatic carriers into early (n=35, <‐10 years) and late (n=22, >‐10 years) groups.First, we performed voxel‐based morphometry (VBM) comparing 24 symptomatic carriers with 32 controls to identify the regions of interest (ROIs) which were atrophic in the symptomatic stage of MAPT. We then used automated and manual segmentations to extract these ROI volumes in all carriers. To remove the effect of age, gender, total intracranial volume and scanner type, we transformed the volumes into w‐scores, considering the controls as the reference group. A w‐score of <‐1.28 (corresponding to the 10th percentile) was considered abnormal.ResultFrom the VBM we identified seven structures significantly atrophic in symptomatic carriers: the nucleus accumbens, amygdala, hippocampus, orbitofrontal cortex, temporal pole, anterior insula and hypothalamus.The percentage of early presymptomatic carriers with abnormal w‐scores was 14% for nucleus accumbens and hippocampus, and 20% orbitofrontal cortex. In the late group, 36% showed abnormal amygdala and temporal pole, 27% abnormal hippocampus, 32% abnormal anterior insula and 9% abnormal hypothalamus. In the symptomatic group, the percentages were higher: nucleus accumbens (41%), amygdala, hippocampus and temporal pole (85%), orbitofrontal cortex (56%), anterior insula (93%) and hypothalamus (48%).ConclusionAbnormal limbic regions are a frequent feature in presymptomatic MAPT carriers, showing early structural changes before symptom onset. Further investigations on the associated cognitive and white matter changes are ongoing.

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