Clinical and neuropathological variability in the rare IVS10 + 14 tau mutation

Selena P. Maxwell; Meghan K. Cash; Kenneth Rockwood; John D. Fisk; Sultan Darvesh

doi:10.1016/j.neurobiolaging.2021.01.004

Clinical and neuropathological variability in the rare IVS10 + 14 tau mutation

Selena P. Maxwell, Meghan K. Cash, Kenneth Rockwood, John D. Fisk, Sultan Darvesh

Résultat de recherche: Article › examen par les pairs

1 Citation (Scopus)

Résumé

Mutations in the microtubule-associated protein tau gene are known to cause progressive neurodegenerative disorders with variable clinical and neuropathological phenotypes, including the intronic 10 + 14 (IVS10 + 14) splice site mutation. Three families have been reported with the IVS10 + 14 microtubule-associated protein tau mutation. Here, we describe the clinical and neuropathological data from an additional family. Neuropathological data were available for 2 of the 3 cases, III-4, and III-5. While III-5 had widespread tau deposition and atrophy, III-4 exhibited more mild neuropathological changes except for the substantia nigra. The previously reported families that express the IVS10 + 14 mutation exhibited significant interfamilial heterogeneity, with symptoms including amyotrophy, dementia, disinhibition, parkinsonism, and breathing problems. In addition to expressing many of these symptoms, members of this fourth family experienced profound sensory abnormalities and sleep disturbance. Although there were probable clinicopathological correlates for the symptoms expressed by the earlier families and III-5 from our cohort, pathology in III-4 did not appear sufficient to explain symptom severity. This indicates the need to explore alternate mechanisms of tau-induced brain dysfunction.

Langue d'origine	English
Pages (de-à)	298.e1-298.e10
Journal	Neurobiology of Aging
Volume	101
DOI	https://doi.org/10.1016/j.neurobiolaging.2021.01.004
Statut de publication	Published - mai 2021

Note bibliographique

Funding Information:
The authors would like to thank Drs Rob Macaulay, Alex Easton, and Sidney Croul for their expertise and assistance in obtaining the neuropathological data in preparation of this article and Kosuke Kanayama for his help with literature translation. This work was supported in part by the Canadian Institutes of Health Research ( PJT- 153319 ), Alzheimer Society of Canada (Research Program Master's Award), Alzheimer Society of Nova Scotia (Phyllis Horton Student Research Award), Dalhousie University Faculty of Medicine (Graduate Studentship), and Dalhousie Medical Research Foundation (Irene MacDonald Sobey Endowed Chair in Curative Approaches to Alzheimer's Disease and The Durland Breakthrough Fund).

Publisher Copyright:
© 2021 Elsevier Inc.

ASJC Scopus Subject Areas

General Neuroscience
Ageing
Developmental Biology
Clinical Neurology
Geriatrics and Gerontology

PubMed: MeSH publication types

Journal Article
Research Support, Non-U.S. Gov't

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10.1016/j.neurobiolaging.2021.01.004

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title = "Clinical and neuropathological variability in the rare IVS10 + 14 tau mutation",

abstract = "Mutations in the microtubule-associated protein tau gene are known to cause progressive neurodegenerative disorders with variable clinical and neuropathological phenotypes, including the intronic 10 + 14 (IVS10 + 14) splice site mutation. Three families have been reported with the IVS10 + 14 microtubule-associated protein tau mutation. Here, we describe the clinical and neuropathological data from an additional family. Neuropathological data were available for 2 of the 3 cases, III-4, and III-5. While III-5 had widespread tau deposition and atrophy, III-4 exhibited more mild neuropathological changes except for the substantia nigra. The previously reported families that express the IVS10 + 14 mutation exhibited significant interfamilial heterogeneity, with symptoms including amyotrophy, dementia, disinhibition, parkinsonism, and breathing problems. In addition to expressing many of these symptoms, members of this fourth family experienced profound sensory abnormalities and sleep disturbance. Although there were probable clinicopathological correlates for the symptoms expressed by the earlier families and III-5 from our cohort, pathology in III-4 did not appear sufficient to explain symptom severity. This indicates the need to explore alternate mechanisms of tau-induced brain dysfunction.",

author = "Maxwell, {Selena P.} and Cash, {Meghan K.} and Kenneth Rockwood and Fisk, {John D.} and Sultan Darvesh",

note = "Funding Information: The authors would like to thank Drs Rob Macaulay, Alex Easton, and Sidney Croul for their expertise and assistance in obtaining the neuropathological data in preparation of this article and Kosuke Kanayama for his help with literature translation. This work was supported in part by the Canadian Institutes of Health Research ( PJT- 153319 ), Alzheimer Society of Canada (Research Program Master's Award), Alzheimer Society of Nova Scotia (Phyllis Horton Student Research Award), Dalhousie University Faculty of Medicine (Graduate Studentship), and Dalhousie Medical Research Foundation (Irene MacDonald Sobey Endowed Chair in Curative Approaches to Alzheimer's Disease and The Durland Breakthrough Fund). Publisher Copyright: {\textcopyright} 2021 Elsevier Inc.",

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Clinical and neuropathological variability in the rare IVS10 + 14 tau mutation

Résumé

Note bibliographique

ASJC Scopus Subject Areas

PubMed: MeSH publication types

Accès au document

Autres fichiers et liens

Empreinte numérique

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