Rare nonsynonymous variants in SORT1 are associated with increased risk for frontotemporal dementia

نویسندگان

  • Stéphanie Philtjens
  • Sara Van Mossevelde
  • Julie van der Zee
  • Eline Wauters
  • Lubina Dillen
  • Mathieu Vandenbulcke
  • Rik Vandenberghe
  • Adrian Ivanoiu
  • Anne Sieben
  • Christiana Willems
  • Luisa Benussi
  • Roberta Ghidoni
  • Giuliano Binetti
  • Barbara Borroni
  • Alessandro Padovani
  • Pau Pastor
  • Monica Diez-Fairen
  • Miquel Aguilar
  • Alexandre de Mendonça
  • Gabriel Miltenberger-Miltényi
  • Isabel Hernández
  • Merce Boada
  • Agustín Ruiz
  • Benedetta Nacmias
  • Sandro Sorbi
  • Maria Rosário Almeida
  • Isabel Santana
  • Jordi Clarimón
  • Alberto Lleó
  • Giovanni B. Frisoni
  • Raquel Sanchez-Valle
  • Albert Lladó
  • Estrella Gómez-Tortosa
  • Ellen Gelpi
  • Marleen Van den Broeck
  • Karin Peeters
  • Patrick Cras
  • Peter P. De Deyn
  • Sebastiaan Engelborghs
  • Marc Cruts
  • Christine Van Broeckhoven
چکیده

We investigated the genetic role of sortilin (SORT1) in frontotemporal dementia (FTD). SORT1 is the neuronal receptor for granulin, encoded by the progranulin gene (GRN), a major causal gene for inherited FTD. In Belgian cohorts of 636 FTD patients and 1066 unaffected control individuals, we identified 5 patient-only nonsynonymous rare variants in SORT1. Rare variant burden analysis showed a significant increase in rare coding variants in patients compared to control individuals (p = 0.04), particularly in the β-propeller domain (p = 0.04), with 2 rare variants located in the predicted binding site for GRN (p = 0.001). We extended these observations by analyzing 3 independent patient/control cohorts sampled in Spain, Italy, and Portugal by partners of the European Early-Onset Dementia Consortium, together with 1155 FTD patients and 1161 control persons. An additional 7 patient-only nonsynonymous variants were observed in SORT1 in European patients. Meta-analysis of the rare nonsynonymous variants in the Belgian and European patient/control cohorts revealed a significant enrichment in FTD patients (p = 0.006), establishing SORT1 as a genetic risk factor for FTD.

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عنوان ژورنال:
  • Neurobiology of aging

دوره   شماره 

صفحات  -

تاریخ انتشار 2018