MRC Centre for Neurodegeneration Research, Institute of Psychiatry, King's College London, London, United Kingdom.
PLoS One. 2011 Feb 25;6(2):e17298. doi: 10.1371/journal.pone.0017298.
Nicastrin is an obligatory component of the γ-secretase; the enzyme complex that leads to the production of Aβ fragments critically central to the pathogenesis of Alzheimer's disease (AD). Analyses of the effects of common variation in this gene on risk for late onset AD have been inconclusive. We investigated the effect of rare variation in the coding regions of the Nicastrin gene in a cohort of AD patients and matched controls using an innovative pooling approach and next generation sequencing. Five SNPs were identified and validated by individual genotyping from 311 cases and 360 controls. Association analysis identified a non-synonymous rare SNP (N417Y) with a statistically higher frequency in cases compared to controls in the Greek population (OR 3.994, CI 1.105-14.439, p = 0.035). This finding warrants further investigation in a larger cohort and adds weight to the hypothesis that rare variation explains some of genetic heritability still to be identified in Alzheimer's disease.
尼卡斯特林是γ-分泌酶的必需成分;这种酶复合物导致 Aβ 片段的产生,这对阿尔茨海默病(AD)的发病机制至关重要。对该基因常见变异对迟发性 AD 风险的影响分析尚无定论。我们使用创新的汇集方法和下一代测序技术,在 AD 患者和匹配对照的队列中研究了尼卡斯特林基因编码区稀有变异的影响。从 311 例病例和 360 例对照中通过个体基因分型鉴定和验证了 5 个 SNP。关联分析确定了一个非同义的罕见 SNP(N417Y),与对照组相比,在希腊人群中的病例中频率更高(OR 3.994,CI 1.105-14.439,p = 0.035)。这一发现需要在更大的队列中进一步研究,并为假设提供了更多依据,即稀有变异解释了一些在阿尔茨海默病中仍有待确定的遗传遗传性。
