AI Article Synopsis

  • Alzheimer's disease is a serious neurodegenerative condition that causes memory loss and cognitive difficulties, ultimately leading to death.
  • Recent studies have identified genetic factors like the APOE epsilon4 allele that contribute to the risk of developing Alzheimer's.
  • In a new genome-wide scan involving 331 patients and 368 controls, no significant new genetic variations were found, but a potential duplication in the CHRNA7 gene may be worth further study.

Article Abstract

Alzheimer's disease is a complex and progressive neurodegenerative disease leading to loss of memory, cognitive impairment, and ultimately death. To date, six large-scale genome-wide association studies have been conducted to identify SNPs that influence disease predisposition. These studies have confirmed the well-known APOE epsilon4 risk allele, identified a novel variant that influences disease risk within the APOE epsilon4 population, found a SNP that modifies the age of disease onset, as well as reported the first sex-linked susceptibility variant. Here we report a genome-wide scan of Alzheimer's disease in a set of 331 cases and 368 controls, extending analyses for the first time to include assessments of copy number variation. In this analysis, no new SNPs show genome-wide significance. We also screened for effects of copy number variation, and while nothing was significant, a duplication in CHRNA7 appears interesting enough to warrant further investigation.

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http://www.ncbi.nlm.nih.gov/pmc/articles/PMC2883723PMC
http://dx.doi.org/10.3233/JAD-2010-1212DOI Listing

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