| Literature DB >> 28888721 |
Nina Rostgaard1, Peter Roos2, Esben Budtz-Jørgensen3, Peter Johannsen1, Gunhild Waldemar1, Anne Nørremølle4, Suzanne G Lindquist5, Susanne Gydesen6, Jeremy M Brown7, John Collinge8, Adrian M Isaacs9, Troels T Nielsen1, Jørgen E Nielsen10.
Abstract
Single-nucleotide polymorphisms in the TMEM106B gene have been identified as a risk factor in frontotemporal dementia (FTD). The major allele of SNP rs3173615 is a risk factor in sporadic FTD, whereas the minor allele seems protective in GRN- and C9orf72-mediated FTD. The role of apolipoprotein E (ApoE) in FTD is uncertain, though an established risk factor in Alzheimer's disease. In a unique Danish family, inherited FTD is caused by a mutation in the CHMP2B gene located on chromosome 3 (FTD-3). In this family, both risk factors TMEM106B and ApoE were analyzed and correlated to age at onset (AAO) and progression in terms of age at institutionalization (AAI) and age at death (AAD). Although TMEM106B and CHMP2B share cellular function in that both localize to endolysosomes, TMEM106B genotypes appeared to have no influence on the clinical disease course. ApoE ε4 was found to be a protective factor with later AAO and AAI, whereas ε2 seemed to aggravate the disease with earlier AAO and AAD. These results indicate ApoE ε2 as a risk factor in FTD-3 and suggest a protective role of ε4.Entities:
Keywords: ApoE; Autosomal dominantly inherited frontotemporal dementia; CHMP2B; FTD-3; SNP rs3173615; TMEM106B
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Year: 2017 PMID: 28888721 DOI: 10.1016/j.neurobiolaging.2017.06.026
Source DB: PubMed Journal: Neurobiol Aging ISSN: 0197-4580 Impact factor: 4.673