Mutation Analysis of Sporadic Early-Onset Alzheimer’s Disease using the NeuroX Array

Mutation Analysis of Sporadic Early-Onset Alzheimer’s Disease using the NeuroX Array

Abstract We have screened sporadic early-onset Alzheimer’s disease (sEOAD, n=408) samples using the NeuroX array for known causative and predicted pathogenic variants in 16 genes linked to familial forms of neurodegeneration. We found two sEOAD individuals harbouring a known causative variant in PAR...

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Veröffentlicht in:Neurobiology of aging 2017-01, Vol.49, p.215.e1-215.e8
Hauptverfasser: Barber, Imelda S, Braae, Anne, Clement, Naomi, Patel, Tulsi, Guetta-Baranes, Tamar, Brookes, Keeley, Medway, Christopher, Chappell, Sally, Guerreiro, Rita, Bras, Jose, Hernandez, Dena, Singleton, Andrew, Hardy, John, Mann, David M, Passmore, Peter, Craig, David, Johnston, Janet, McGuinness, Bernadette, Todd, Stephen, Heun, Reinhard, Kölsch, Heike, Kehoe, Patrick G, Vardy, Emma R.L.C, Hooper, Nigel M, Pickering-Brown, Stuart, Snowden, Julie, Richardson, Anna, Jones, Matthew, Neary, David, Harris, Jennifer, Lowe, James, Smith, A. David, Wilcock, Gordon, Warden, Donald, Holmes, Clive, Morgan, Kevin
Format: Artikel
Sprache:eng
Schlagworte:
Alzheimer Disease - genetics
Alzheimer's disease
DNA Mutational Analysis - methods
Early-onset
Genetic Association Studies
Genetic Predisposition to Disease - genetics
Genetic Testing
Genetic Variation - genetics
Humans
Internal Medicine
Neurology
NeuroX
Oligonucleotide Array Sequence Analysis - methods
Parkinson Disease - genetics
Parkinson's disease
Screening
Sporadic
tau Proteins - genetics
Ubiquitin-Protein Ligases - genetics
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Zusammenfassung:Abstract We have screened sporadic early-onset Alzheimer’s disease (sEOAD, n=408) samples using the NeuroX array for known causative and predicted pathogenic variants in 16 genes linked to familial forms of neurodegeneration. We found two sEOAD individuals harbouring a known causative variant in PARK2 known to cause early-onset Parkinson’s disease (EOPD); p.T240M (n=1) and p.Q34fs delAG (n=1). Additionally, we identified three sEOAD individuals harbouring a predicted pathogenic variant in MAPT (p.A469T) which has previously been associated with AD. It is currently unknown if these variants affect susceptibility to sEOAD, further studies would be needed to establish this. This work highlights the need to screen sEOAD individuals for variants that are more classically attributed to other forms of neurodegeneration.
ISSN:0197-4580
1558-1497
DOI:10.1016/j.neurobiolaging.2016.09.008