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Dissemination in time and space in presymptomatic granulin mutation carriers: a GENFI spatial chronnectome study

Authors :
Sandro Sorbi
Vince D. Calhoun
James B. Rowe
Isabelle Le Ber
Matthis Synofzik
Roberto Gasparotti
Martina Bocchetta
Enrico Premi
Dave Cash
Alexandre de Mendonça
Armin Iraji
Johannes Levin
Stefano Gazzina
A. Danek
Lize C. Jiskoot
Marcello Giunta
Alexander Gerhard
Markus Otto
Raquel Sánchez-Valle
Emily Todd
Genetic Frontotemporal dementia Initiative
Isabel Santana
Silvana Archetti
Rhian S Convery
Robert Laforce
Srinivas Rachakonda
Florence Pasquier
Fermin Moreno
John C. van Swieten
Georgia Peakman
Elizabeth Finger
Jonathan D. Rohrer
Christopher C Butler
Daniela Galimberti
Alberto Benussi
Carmela Tartaglia
Rik Vandenberghe
Caroline Graff
Mario Masellis
Fabrizio Tagliavini
Barbara Borroni
Simon Ducharme
Genetic Frontotemporal dementia Initiative (GENFI)
Neurology
Clinical Genetics
Source :
Neurobiology of Aging, 108, 155-167. Elsevier Inc.
Publication Year :
2021
Publisher :
Elsevier BV, 2021.

Abstract

The presymptomatic brain changes of granulin (GRN) disease, preceding by years frontotemporal dementia, has not been fully characterized. New approaches focus on the spatial chronnectome can capture both spatial network configurations and their dynamic changes over time. To investigate the spatial dynamics in 141 presymptomatic GRN mutation carriers and 282 noncarriers from the Genetic Frontotemporal dementia research Initiative cohort. We considered time-varying patterns of the default mode network, the language network, and the salience network, each summarized into 4 distinct recurring spatial configurations. Dwell time (DT) (the time each individual spends in each spatial state of each network), fractional occupacy (FO) (the total percentage of time spent by each individual in a state of a specific network) and total transition number (the total number of transitions performed by each individual in a specifict state) were considered. Correlations between DT, FO, and transition number and estimated years from expected symptom onset (EYO) and clinical performances were assessed. Presymptomatic GRN mutation carriers spent significantly more time in those spatial states characterised by greater activation of the insula and the parietal cortices, as compared to noncarriers (p < 0.05, FDR-corrected). A significant correlation between DT and FO of these spatial states and EYO was found, the longer the time spent in the spatial states, the closer the EYO. DT and FO significantly correlated with performances at tests tapping processing speed, with worse scores associated with increased spatial states’ DT. Our results demonstrated that presymptomatic GRN disease presents a complex dynamic reorganization of brain connectivity. Change in both the spatial and temporal aspects of brain network connectivity could provide a unique glimpse into brain function and potentially allowing a more sophisticated evaluation of the earliest disease changes and the understanding of possible mechanisms in GRN disease.

Details

ISSN :
01974580
Volume :
108
Database :
OpenAIRE
Journal :
Neurobiology of Aging
Accession number :
edsair.doi.dedup.....8b8e506d618663e4dcc4d5c48192a94c