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KIBRA genetic polymorphism influences episodic memory in later life but does not increase the risk of mild cognitive impairment

机译:KIBRA基因多态性影响晚年的情景记忆但不会增加轻度认知障碍的风险

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摘要

A common T→C polymorphism of the KIBRA gene has been recently associated with worse performance on tests of episodic memory. This should aimed to determine whether older adults with the KIBRA CC genotype (1) have worse episodic memory than T-allele carriers and, (2) are more likely to express the phenotype of amnestic mild cognitive impairment (MCI). Our Cross-sectional investigation of 312 adults aged 50–89 years free of dementia included genotyping of the KIBRA rs17070145 gene and the assessment of episodic memory to Establish a Registry for Alzheimer's Disease (CERAD). Participants were considered to have MCI if their memory scores were 1.5 standard deviations below the mean norm for the population. 138/312 participants carried the KIBRA CC genotype. Their immediate and delayed recall scores were significantly lower than the scores of carriers of the T allele (P < 0.05; adjusted for age, gender and pre-morbid IQ), although the effect size of the CC genotype was weak (0.2). Amongst our volunteers, 133 had MCI, of whom 63 (47.4%) had the CC genotype. There was no association between KIBRA genotype and MCI phenotype (TT/CT versus CC; adjusted odds ratio = 1.70, 95%CI = 0.74, 3.90). We concluded that the KIBRA T→C polymorphism contributes to modulate episodic memory amongst community-dwelling older adults free of dementia, but plays no obvious role in the phenotypic expression of MCI. Future studies should aim to clarify the long term implications of this polymorphism on cognitive function and to identify other genes involved in the modulation of memory that might confer greater risk of MCI in later life.
机译:KIBRA基因的常见T→C多态性最近与情景记忆测试中的较差性能有关。这应该旨在确定具有KIBRA CC基因型的老年人(1)是否具有比T等位基因携带者更差的情节记忆,以及(2)更可能表现出轻度轻度认知障碍(MCI)的表型。我们对312位50-89岁无痴呆症的成年人进行了横断面调查,包括KIBRA rs17070145基因的基因分型和对情景记忆的评估,以建立阿尔茨海默氏病(CERAD)注册表。如果参与者的记忆力得分低于总体平均标准1.5个标准差,则认为他们患有MCI。 138/312名参与者携带了KIBRA CC基因型。尽管CC基因型的影响大小较弱(0.2),但他们的即时和延迟回忆得分显着低于T等位基因携带者的得分(P <0.05;根据年龄,性别和病前智商进行调整)。在我们的志愿者中,有133名患有MCI,其中63名(47.4%)具有CC基因型。 KIBRA基因型和MCI表型之间没有关联(TT / CT与CC;调整后的优势比= 1.70,95%CI = 0.74,3.90)。我们得出的结论是,KIBRA T→C多态性有助于调节无痴呆的社区居民老年人的情节记忆,但在MCI的表型表达中没有明显作用。未来的研究应旨在阐明这种多态性对认知功能的长期影响,并确定与记忆调节有关的其他基因,这些基因可能在以后的生活中增加MCI的风险。

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