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Rare mutations in SQSTM1 modify susceptibility to frontotemporal lobar degeneration
der Zee J van, Langenhove T Van, GG Kovacs, L Dillen, W Deschamps, S Engelborghs, R Matej, M Vandenbulcke, A Sieben, B Dermaut, K Smets, Damme P Van, C Merlin, A Laureys, Den Broeck M Van, M Mattheijssens, K Peeters, L Benussi, G Binetti, R...
Jazyk angličtina Země Německo
Grantová podpora
NT12094
MZ0
CEP - Centrální evidence projektů
Digitální knihovna NLK
Plný text - Článek
Zdroj
NLK
ProQuest Central
od 1997-01-01 do Před 1 rokem
Health & Medicine (ProQuest)
od 1997-01-01 do Před 1 rokem
Psychology Database (ProQuest)
od 1997-01-01 do Před 1 rokem
- MeSH
- adaptorové proteiny signální transdukční * genetika MeSH
- amyotrofická laterální skleróza MeSH
- DNA vazebné proteiny genetika MeSH
- dospělí MeSH
- frontotemporální lobární degenerace * genetika patologie MeSH
- genetická predispozice k nemoci * genetika MeSH
- jednonukleotidový polymorfismus * genetika MeSH
- kohortové studie MeSH
- lidé středního věku MeSH
- lidé MeSH
- metaanalýza jako téma MeSH
- mezinárodní spolupráce MeSH
- mutační analýza DNA MeSH
- sekvestosom 1 MeSH
- senioři nad 80 let MeSH
- senioři MeSH
- zvířata MeSH
- Check Tag
- dospělí MeSH
- lidé středního věku MeSH
- lidé MeSH
- mužské pohlaví MeSH
- senioři nad 80 let MeSH
- senioři MeSH
- ženské pohlaví MeSH
- zvířata MeSH
Mutations in the gene coding for Sequestosome 1 (SQSTM1) have been genetically associated with amyotrophic lateral sclerosis (ALS) and Paget disease of bone. In the present study, we analyzed the SQSTM1 coding sequence for mutations in an extended cohort of 1,808 patients with frontotemporal lobar degeneration (FTLD), ascertained within the European Early-Onset Dementia consortium. As control dataset, we sequenced 1,625 European control individuals and analyzed whole-exome sequence data of 2,274 German individuals (total n = 3,899). Association of rare SQSTM1 mutations was calculated in a meta-analysis of 4,332 FTLD and 10,240 control alleles. We identified 25 coding variants in FTLD patients of which 10 have not been described. Fifteen mutations were absent in the control individuals (carrier frequency <0.00026) whilst the others were rare in both patients and control individuals. When pooling all variants with a minor allele frequency <0.01, an overall frequency of 3.2 % was calculated in patients. Rare variant association analysis between patients and controls showed no difference over the whole protein, but suggested that rare mutations clustering in the UBA domain of SQSTM1 may influence disease susceptibility by doubling the risk for FTLD (RR = 2.18 [95 % CI 1.24-3.85]; corrected p value = 0.042). Detailed histopathology demonstrated that mutations in SQSTM1 associate with widespread neuronal and glial phospho-TDP-43 pathology. With this study, we provide further evidence for a putative role of rare mutations in SQSTM1 in the genetic etiology of FTLD and showed that, comparable to other FTLD/ALS genes, SQSTM1 mutations are associated with TDP-43 pathology.
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