Anomia is present pre-symptomatically in frontotemporal dementia due to MAPT mutations

Arabella Bouzigues ,Catharina Prix ,Carlo Wilke ,Paola Caroppo ,Marta Cañada ,Giorgio Fumagalli ,Sandra E Black ,Serge Gauthier ,Jorge Villanúa ,Imogen J Swift ,Myriam Barandiarán ,Aurélie Funkiewiez ,Martina Bocchetta ,Giacomina Rossi ,Anne Bertrand ,Tobias Langheinrich ,Gabriel Miltenberger ,Jackie M Poos ,David F Tang‐Wai ,Benjamín Bender ,Annerose Engel ,Valentina Bessi ,Linn Öijerstedt ,Vesna Jelić ,Chiara Fenoglio ,Alexander Gerhard ,Simon Ducharme ,Agnès Camuzat ,Rick Van Minkelen ,Isabel Santana ,Timothy Rittman ,Sergi Borrego‐Écija ,Isabelle Le Ber ,Maxime Bertoux ,Alazne Gabilondo ,Maria João Leitão ,Sonja Schönecker ,Rhian S Convery ,Pietro Tiraboschi ,Catarina Ferreira ,Elisabeth Wlasich ,Olivia Wagemann ,Carolyn Timberlake ,Ron Keren ,Sandro Sorbi ,Sara Prioni ,Henrik Zetterberg ,Jolina Lombardi ,Miguel Castelo‐Branco ,David M Cash ,Dario Saracino ,John Van Swieten ,Tobias Hoegen ,Sónia Afonso ,Grégory Kuchcinski ,Maria Rosário Almeida ,Rachelle Shafei ,Elizabeth Finger ,Alberto Benussi ,Joaquı́n Castilla ,Andrea Arighi ,Gemma Lombardi ,Christen Shoesmith ,Lucia Giannini ,Robart Bartha ,Barbara Borroni ,Robert Laforce ,Paul M Thompson ,Adrian Danek ,Carolin Heller ,Silvana Archetti ,Giorgio Giaccone ,Frederico Simões Do Couto ,Rik Vandenberghe ,Pedro Rosa‐Neto ,Sandra Loosli ,Patricia Alves ,Caroline Graff ,Valentina Cantoni ,Diana Duro ,Mircea Balasa ,Annabel Nelson ,Sara Mitchell ,Alexandre De Mendonça ,Janne M Papma ,Maria Carmela Tartaglia ,Lucy L Russell ,Núria Bargalló ,Chris Butler ,Lisa Graf ,Chengjie Xiong ,Hanya Benotmane ,Sabrina Sayah ,Beatriz Santiago ,Rosa Rademakers ,Roberto Gasparotti ,Koen Poesen ,Caroline Greaves ,Vincent Deramecourt ,Miren Zulaica ,Markus Otto ,Albert Lladò ,Harro Seelaar ,Daisy Rinaldi ,Mikel Tainta ,Camilla Ferrari ,Stefano Gazzina ,Ana Verdelho ,Matthis Synofzik ,Enrico Premi ,Daniela Galimberti ,Thomas Cope ,Fermín Moreno ,Veronica Redaelli ,Sarah Anderl‐Straub ,Adeline Rollin ,James B Rowe ,Florence Pasquier ,Carolina Maruta ,Yolande A.l Pijnenburg ,Mario Masellis ,Anna Antonell ,Benedetta Nacmias ,Rose Bruffaerts ,Kiran Samra ,Vittoria Borracci ,Elio Scarpini ,Alexis Brice ,Olivier Colliot ,Aitana Sogorb‐Esteve ,Jaume Olives ,Michele Veldsman ,Jennifer M Nicholas ,David L Thomas ,Cristina Polito ,Emily Todd ,Christin Andersson ,Annick Vogels ,Jonathan D Rohrer ,Mathieu Vandenbulcke ,Ana Gorostidi ,Ekaterina Rogaeva ,Philip Van Damme ,Håkan Thonberg ,Thibaud Lebouvier ,Georgia Peakman ,Miguel Tábuas‐Pereira ,Lize C Jiskoot ,Maryna Polyakova

doi:10.1007/s00415-022-11068-0

Abstract

IntroductionA third of frontotemporal dementia (FTD) is caused by an autosomal-dominant genetic mutation in one of three genes: microtubule-associated protein tau (MAPT), chromosome 9 open reading frame 72 (C9orf72) and progranulin (GRN). Prior studies of prodromal FTD have identified impaired executive function and social cognition early in the disease but few have studied naming in detail.MethodsWe investigated performance on the Boston Naming Test (BNT) in the GENetic Frontotemporal dementia Initiative cohort of 499 mutation carriers and 248 mutation-negative controls divided across three genetic groups: C9orf72, MAPT and GRN. Mutation carriers were further divided into 3 groups according to their global CDR plus NACC FTLD score: 0 (asymptomatic), 0.5 (prodromal) and 1 + (fully symptomatic). Groups were compared using a bootstrapped linear regression model, adjusting for age, sex, language and education. Finally, we identified neural correlates of anomia within carriers of each genetic group using a voxel-based morphometry analysis.ResultsAll symptomatic groups performed worse on the BNT than controls with the MAPT symptomatic group scoring the worst. Furthermore, MAPT asymptomatic and prodromal groups performed significantly worse than controls. Correlates of anomia in MAPT mutation carriers included bilateral anterior temporal lobe regions and the anterior insula. Similar bilateral anterior temporal lobe involvement was seen in C9orf72 mutation carriers as well as more widespread left frontal atrophy. In GRN mutation carriers, neural correlates were limited to the left hemisphere, and involved frontal, temporal, insula and striatal regions.ConclusionThis study suggests the development of early anomia in MAPT mutation carriers, likely to be associated with impaired semantic knowledge. Clinical trials focused on the prodromal period within individuals with MAPT mutations should use language tasks, such as the BNT for patient stratification and as outcome measures.

Full Text