Naomi Clement
Investigating splicing variants uncovered by next-generation sequencing the Alzheimer’s disease candidate genes, CLU, PICALM, CR1, ABCA7, BIN1, the MS4A locus, CD2AP, EPHA1 and CD33
Clement, Naomi; Braae, Anne; Turton, James; Lord, Jenny; Guetta-Baranes, Tamar; Medway, Christopher; Brookes, Keeley; Barber, Imelda S.; Patel, Tulsi; Milla, Lucy; Azzopardi, Maria; Lowe, James; Mann, David; Pickering-Brown, Stuart; Kalsheker, Noor; Passmore, Peter; Chappell, Sally; Morgan, Kevin
Authors
Anne Braae
James Turton
Jenny Lord
Tamar Guetta-Baranes
Christopher Medway
Keeley Brookes
Imelda S. Barber
Tulsi Patel
Lucy Milla
Maria Azzopardi
James Lowe
David Mann
Stuart Pickering-Brown
Noor Kalsheker
Peter Passmore
Sally Chappell
Kevin Morgan
Abstract
Late onset Alzheimer’s disease (LOAD), the most common cause of late onset dementia, has a strong genetic component. To date, 21 disease-risk loci have been identified through genome wide association studies (GWAS). However, the causative functional variant(s) within these loci are yet to be discovered. This study aimed to identify potential functional splicing mutations in the nine original GWAS-risk genes: CLU, PICALM, CR1, ABCA7, BIN1, the MS4A locus, CD2AP, EPHA1 and CD33. Target enriched next generation sequencing (NGS) was used to resequence the entire genetic region for each of these GWAS-risk loci in 96 LOAD patients and in silico databases were used to annotate the variants for functionality. Predicted splicing variants were further functionally characterised using splicing prediction software and minigene splicing assays. Following in silico annotation, 21 variants were predicted to influence splicing and, upon further annotation, four of these were examined utilising the in vitro minigene assay. Two variants, rs881768 A>G in ABCA7 and a novel variant 11: 60179827 T>G in MS4A6A were shown, in these cell assays, to affect the splicing of these genes. The method employed in the paper successfully identified potential splicing variants in GWAS-risk genes. Further investigation will be needed to understand the full effect of these variants on LOAD risk. However, these results suggest a possible pipeline in order to identify putative functional variants as a result of NGS in disease-associated loci although improvements are needed within the current prediction programme in order to reduce the number of false positives.
Citation
Clement, N., Braae, A., Turton, J., Lord, J., Guetta-Baranes, T., Medway, C., Brookes, K., Barber, I. S., Patel, T., Milla, L., Azzopardi, M., Lowe, J., Mann, D., Pickering-Brown, S., Kalsheker, N., Passmore, P., Chappell, S., & Morgan, K. (in press). Investigating splicing variants uncovered by next-generation sequencing the Alzheimer’s disease candidate genes, CLU, PICALM, CR1, ABCA7, BIN1, the MS4A locus, CD2AP, EPHA1 and CD33. Journal of Alzheimer's Disease and Parkinsonism, 6(6), https://doi.org/10.4172/2161-0460.1000276
Journal Article Type | Article |
---|---|
Acceptance Date | Oct 22, 2016 |
Online Publication Date | Oct 29, 2016 |
Deposit Date | Nov 2, 2016 |
Publicly Available Date | Nov 2, 2016 |
Journal | Journal of Alzheimers Disease & Parkinsonism |
Electronic ISSN | 2161-0460 |
Publisher | OMICS International |
Peer Reviewed | Peer Reviewed |
Volume | 6 |
Issue | 6 |
DOI | https://doi.org/10.4172/2161-0460.1000276 |
Keywords | Late onset Alzheimer’s disease; Next generation sequencing; Splicing; Annotation; Functional variations; Minigene assays |
Public URL | https://nottingham-repository.worktribe.com/output/821019 |
Publisher URL | https://www.omicsonline.org/open-access/investigating-splicing-variants-uncovered-by-nextgeneration-sequencingthe-alzheimers-disease-candidate-genes-clu-picalm-cr1-abca7b-2161-0460-1000276.php?aid=82714 |
Contract Date | Nov 2, 2016 |
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Copyright Statement
Copyright information regarding this work can be found at the following address: http://creativecommons.org/licenses/by/4.0
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