Heritability in frontotemporal tauopathies

Shelley L. Forrest; Glenda M. Halliday; Heather McCann; Andrew B. McGeachie; Ciara V. McGinley; John R. Hodges; Olivier Piguet; John B. Kwok; Maria G. Spillantini; Jillian J. Kril

doi:10.1016/j.dadm.2018.12.001

Alzheimer’s & Dementia: Diagnosis, Assessment & Disease Monitoring (Dec 2019)

Heritability in frontotemporal tauopathies

Shelley L. Forrest,
Glenda M. Halliday,
Heather McCann,
Andrew B. McGeachie,
Ciara V. McGinley,
John R. Hodges,
Olivier Piguet,
John B. Kwok,
Maria G. Spillantini,
Jillian J. Kril

Affiliations

Shelley L. Forrest: Faculty of Medicine and Health, Charles Perkins Centre and Discipline of PathologyUniversity of SydneySydneyAustralia
Glenda M. Halliday: Faculty of Medicine and HealthBrain and Mind Centre and Central Clinical School, University of SydneySydneyAustralia
Heather McCann: Neuroscience Research AustraliaSydneyAustralia
Andrew B. McGeachie: Neuroscience Research AustraliaSydneyAustralia
Ciara V. McGinley: Faculty of Medicine and Health, Charles Perkins Centre and Discipline of PathologyUniversity of SydneySydneyAustralia
John R. Hodges: Faculty of Medicine and HealthBrain and Mind Centre and Central Clinical School, University of SydneySydneyAustralia
Olivier Piguet: Neuroscience Research AustraliaSydneyAustralia
John B. Kwok: Faculty of Medicine and HealthBrain and Mind Centre and Central Clinical School, University of SydneySydneyAustralia
Maria G. Spillantini: Department of Clinical NeurosciencesUniversity of CambridgeCambridgeUK
Jillian J. Kril: Faculty of Medicine and Health, Charles Perkins Centre and Discipline of PathologyUniversity of SydneySydneyAustralia

DOI: https://doi.org/10.1016/j.dadm.2018.12.001
Journal volume & issue: Vol. 11, no. 1
pp. 115 – 124

Abstract

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Abstract Introduction Exploring the degree of heritability in a large cohort of frontotemporal lobar degeneration with tau‐immunopositive inclusions (FTLD‐tau) and determining if different FTLD‐tau subtypes are associated with stronger heritability will provide important insight into disease pathogenesis. Methods Using modified Goldman pedigree classifications, heritability was examined in pathologically proven FTLD‐tau cases with dementia at any time (n = 124) from the Sydney‐Cambridge collection. Results Thirteen percent of the FTLD‐tau cohort have a suggested autosomal dominant pattern of inheritance, 25% have some family history, and 62% apparently sporadic. MAPT mutations were found in 9% of cases. Globular glial tauopathy was associated with the strongest heritability with 40% having a suggested autosomal dominant pattern of inheritance followed by corticobasal degeneration (19%), Pick's disease (8%), and progressive supranuclear palsy (6%). Discussion Similar to clinical frontotemporal dementia syndromes, heritability varies between pathological subtypes. Further identification of a genetic link in cases with strong heritability await discovery.

Published in Alzheimer’s & Dementia: Diagnosis, Assessment & Disease Monitoring

ISSN: 2352-8729 (Online)
Publisher: Wiley
Country of publisher: United States
LCC subjects: Medicine: Internal medicine: Neurosciences. Biological psychiatry. Neuropsychiatry: Neurology. Diseases of the nervous system; Medicine: Internal medicine: Special situations and conditions: Geriatrics
Website: https://alz-journals.onlinelibrary.wiley.com/journal/23528729

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