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Possible positive effect of the APOE ε2 allele on cognition in early to mid-adult life

机译:APOEε2等位基因可能对成年早期和中期的认知产生积极影响

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摘要

Backgroundε4 allele possession is associated with an increased risk of Alzheimer’s disease. Its effects earlier in life are less well understood. Previous studies have reported both detrimental effects and a lack of effect on cognition outside dementia. We used genotype based recall from the ALSPAC study to investigate whether APOE genotype influences cognition in earlier adult life.MethodsWe invited all individuals with the rarer ε22 or ε44 genotypes and equal numbers of those with ε32, ε33 or ε34 APOE genotypes (total n invited =1936, ages 23-67). Participants were screened for dementia using the Addenbrooke’s Cognitive Examination Revised (ACE-R). Participants were asked to complete a 3 hour battery of neuropsychological tests covering a range of cognitive domains. The primary outcome was performance on the Rey Auditory Verbal Learning Test (RAVLT). Transformation of variables was used where required to permit parametric testing. As genotypes are unlikely to be confounded unadjusted analyses were performed.Results114 participants were recruited to the study (39 ε33, 27 ε34, 15 ε44, 26 ε32 & 7 ε22). ε4+ participants had higher scores on the cognitive failures questionnaire (10 point increase, p=0.006) but no deficits on objective cognitive testing. ε2 carriers had slightly better episodic memory performance (p=0.016), slightly improved n-back accuracy and better executive functioning (trails A&B, p=0.005). ConclusionsIt is intriguing that the ε2+ group performed better as this group have a lower risk of Alzheimer’s disease. Most previous studies have analysed as ε4/non ε4 so may have missed this effect.
机译:背景ε4等位基因的占有与阿尔茨海默氏病风险增加有关。人们对生命早期的影响了解得很少。先前的研究已经报道了痴呆之外的有害影响和对认知的缺乏。我们使用来自ALSPAC研究的基于基因型的回忆来研究APOE基因型是否会影响成年早期的认知。方法我们邀请了所有具有ε22或ε44基因型罕见的个体以及平等数量的ε32,ε33或ε34APOE基因型的个体(被邀请的总n = 1936年,年龄在23-67岁之间。使用Addenbrooke的认知检查修订版(ACE-R)对参与者进行了痴呆症筛查。要求参与者完成3小时的神经心理学测试,涵盖一系列认知领域。主要结果是雷伊听觉语言学习测验(RAVLT)的表现。在允许进行参数测试的地方使用了变量的转换。由于不容易混淆基因型,因此未经校正的分析未进行。结果招募了114名参与者(39 ε33、27 ε34、15 ε44、26ε32和7ε22)。 ε4+参与者在认知障碍问卷上得分较高(增加10分,p = 0.006),但客观认知测试无缺陷。 ε2载体的情节记忆性能稍好(p = 0.016),n背准确性稍高,执行功能更好(轨迹A&B,p = 0.005)。结论有趣的是ε2+组表现更好,因为该组患阿尔茨海默氏病的风险较低。先前的大多数研究都将其分析为ε4/非ε4,因此可能错过了这种影响。

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