Searching for just a few words should be enough to get started. If you need to make more complex queries, use the tips below to guide you.
Article type: Research Article
Authors: Boada, Mercèa; b | Antúnez, Carmenc; d | López-Arrieta, Jesúse | Galán, José Jorgef | Morón, Francisco J.f | Hernández, Isabela | Marín, Juanc | Martínez-Lage, Pabloa | Alegret, Montserrata | Carrasco, Jose M.f | Moreno, Conchaf | Real, Luis M.f | González-Pérez, Antoniof | Tárraga, Lluísa; b | Ruiz, Agustínf; *
Affiliations: [a] Memory Clinic of Fundació ACE. Institut Català de Neurociencies Aplicades, Barcelona, Spain | [b] Neurology Service, University General Hospital Vall d'Hebron, Barcelona, Spain | [c] Dementia Unit, University Hospital Virgen de la Arrixaca, Murcia, Spain | [d] Alzheimur Foundation, Murcia, Spain | [e] Memory Unit, University Hospital La Paz-Cantoblanco, Madrid, Spain | [f] Department of Structural Genomics, NeoCodex, Sevilla, Spain
Correspondence: [*] Correspondence to: Dr. Agustín Ruiz, Department of Structural Genomics, Neocodex SL, Avda. Charles Darwin 6, Acceso A. Parque Científico y Tecnológico Isla de la Cartuja, 41092-Seville, Spain. Tel.: +34 657816907; Fax: +34 955047325; E-mail: [email protected].
Note: [] Handling Associate Editor: Weixiong Zhang
Abstract: CALHM1 gene coding non-synonymous SNP P86L (rs2986017) was reported to increase the risk of Alzheimer's disease (AD) in a recent study. We have investigated this genetic variant in 2470 individuals from Spain to conduct an independent replication study of the proposed SNP marker. By applying a recessive model, we observed weak evidence of an association between P86L mutation and late-onset AD (LOAD) susceptibility in our case-control study (OR = 1.38 C.I. = [1.01–1.89]). Meta-analysis of available studies also supports a recessive model for CALHM1 P86L variant and provides evidence of between study heterogeneity. Importantly, we found that adjusted mean age at AD onset in P86L homozygous LOAD patients was significantly earlier that in the rest of patients (77.01 ± 6.1 for P86L homozygous carriers versus 79.0 ± 6.0 for the rest of patients, p = 0.002). We concluded that the CALMH1 gene may contribute to AD risk in our study population. The observed genetic model (recessive) and the estimated magnitude of the effect both imply that virtually all studies performed to date were markedly underpowered to detect this effect and underscore the importance of follow up, replication, and meta-analyses of promising genetic signals.
Keywords: Alzheimer's disease, association, CALHM1, genotype, meta-analysis, molecular genetics, polymorphism
DOI: 10.3233/JAD-2010-1357
Journal: Journal of Alzheimer's Disease, vol. 20, no. 1, pp. 247-251, 2010
IOS Press, Inc.
6751 Tepper Drive
Clifton, VA 20124
USA
Tel: +1 703 830 6300
Fax: +1 703 830 2300
[email protected]
For editorial issues, like the status of your submitted paper or proposals, write to [email protected]
IOS Press
Nieuwe Hemweg 6B
1013 BG Amsterdam
The Netherlands
Tel: +31 20 688 3355
Fax: +31 20 687 0091
[email protected]
For editorial issues, permissions, book requests, submissions and proceedings, contact the Amsterdam office [email protected]
Inspirees International (China Office)
Ciyunsi Beili 207(CapitaLand), Bld 1, 7-901
100025, Beijing
China
Free service line: 400 661 8717
Fax: +86 10 8446 7947
[email protected]
For editorial issues, like the status of your submitted paper or proposals, write to [email protected]
如果您在出版方面需要帮助或有任何建, 件至: [email protected]