A family with tau-negative frontotemporal dementia and neuronal intranuclear inclusions linked to chromosome 17

Ian R. Mackenzie , Matthew Baker , Gemma West , Ian R. Mackenzie , Matthew Baker , Gemma West , John Woulfe , Najeeb Qadi , Jennifer Gass , Ashley Cannon , Jennifer Adamson , Howard Feldman , Caroline Lindholm , Stacey Melquist , Rachel Pettman , A. Dessa Sadovnick , Emily Dwosh , Sidney W. Whiteheart , Michael Hutton , Stuart Pickering‐Brown
2006 Brain 104 citations

Abstract

Over 30 different mutations have now been identified in MAPt that cause frontotemporal dementia (FTD). However, there are several families with FTD that show definite linkage to the region on chromosome 17 that contains MAPt, in which no mutation(s) has been identified. Although these families could have a complex mutation of the MAPt locus that has evaded detection it is also possible that another gene in this region is associated with FTD. This possibility is supported by neuropathological findings in these families, which consist of neuronal inclusions that are immunoreactive for ubiquitin (ub-ir) but not for tau. In addition to neuronal cytoplasmic inclusions, several chromosome 17-linked families are reported to have ub-ir neuronal intranuclear inclusions (NII); a finding which is uncommon in sporadic FTD. Here, we describe detailed clinical and neuropathological findings in a new large, multigenerational family with autosomal dominant FTD and autopsy proven tau-negative, ub-ir neuronal cytoplasmic and intranuclear inclusions. We have demonstrated that this family is linked to a 19.06 cM region of chromosome 17q21 with a maximum multipoint LOD score of 3.911 containing MAPt. By combining the results of our genetic analysis with those previously published for other families with similar pathology, we have further refined the minimal region to a 3.53 cM region of chromosome 17q21. We did not identify point mutations in MAPt by direct sequencing or any gross MAPt gene alterations using fluorescent in situ hybridization. In addition, tau protein extracted from members of this family was unremarkable in size and quantity as assessed by western blotting. Neuropathological characterization of the ub-ir NII in this family shows that they are positive for promyelocytic leukaemia protein (PML) and SUMO-1 that suggests that these inclusions form in the nuclear body and suggests a possible mechanism of neurodegeneration in tau-negative FTD linked to chromosome 17q21.

Keywords

Frontotemporal dementiaTau proteinChromosome 17 (human)BiologyLocus (genetics)Chromosome 22GeneticsGenetic linkagePathologyDementiaChromosomeGeneAlzheimer's diseaseMedicineDisease

MeSH Terms

AgedBlottingWesternChromosomesHumanPair 17DementiaFemaleGenetic LinkageGenetic Predisposition to DiseaseHumansIn Situ HybridizationFluorescenceIntranuclear Inclusion BodiesMaleMiddle AgedNeuronsPedigreeUbiquitintau Proteins

Related Publications

Publication Info

Year
2006
Type
article
Volume
129
Issue
4
Pages
853-867
Citations
104
Access
Closed

External Links

Download PDF (Free) View on DOI.org PubMed Semantic Scholar

Social Impact

Altmetric
PlumX Metrics

Social media, news, blog, policy document mentions

Citation Metrics

104
OpenAlex
4
Influential
75
CrossRef

Cite This

Ian R. Mackenzie, Matthew Baker, Gemma West et al. (2006). A family with tau-negative frontotemporal dementia and neuronal intranuclear inclusions linked to chromosome 17. Brain , 129 (4) , 853-867. https://doi.org/10.1093/brain/awh724

Identifiers

DOI
10.1093/brain/awh724
PMID
16401619

Data Quality

Data completeness: 90%