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研究KIBRA和CLSTN2基因多态性对老年人记忆表现和海马体体积的横断面及纵向测量指标的影响。

Investigating the influence of KIBRA and CLSTN2 genetic polymorphisms on cross-sectional and longitudinal measures of memory performance and hippocampal volume in older individuals.

作者信息

Boraxbekk C J, Ames David, Kochan Nicole A, Lee Teresa, Thalamuthu Anbupalam, Wen Wei, Armstrong Nicola J, Kwok John B J, Schofield Peter R, Reppermund Simone, Wright Margaret J, Trollor Julian N, Brodaty Henry, Sachdev Perminder, Mather Karen A

机构信息

CEDAR, Center for Demographic and Aging Research, Umeå University, S-901 87 Umeå, Sweden; UFBI, Umeå centre for Functional Brain Imaging, Umeå University, Sweden.

National Ageing Research Institute, Parkville, Victoria, Australia; Department of Psychiatry, University of Melbourne, Victoria, Australia.

出版信息

Neuropsychologia. 2015 Nov;78:10-7. doi: 10.1016/j.neuropsychologia.2015.09.031. Epub 2015 Sep 28.

Abstract

The variability of episodic memory decline and hippocampal atrophy observed with increasing age may partly be explained by genetic factors. KIBRA (kidney and brain expressed protein) and CLSTN2 (calsyntenin 2) are two candidate genes previously linked to episodic memory performance and volume of the hippocampus, a key memory structure. However, whether polymorphisms in these two genes also influence age-related longitudinal memory decline and hippocampal atrophy is still unknown. Using data from two independent cohorts, the Sydney Memory and Ageing Study and the Older Australian Twins Study, we investigated whether the KIBRA and CLSTN2 genetic polymorphisms (rs17070145 and rs6439886) are associated with episodic memory performance and hippocampal volume in older adults (65-90 years at baseline). We were able to examine these polymorphisms in relation to memory and hippocampal volume using cross-sectional data and, more importantly, also using longitudinal data (2 years between testing occasions). Overall we did not find support for an association of KIBRA either alone or in combination with CLSTN2 with memory performance or hippocampal volume, nor did variation in these genes influence longitudinal memory decline or hippocampal atrophy in two cohorts of older adults.

摘要

随着年龄增长观察到的情景记忆衰退和海马萎缩的变异性,可能部分由遗传因素解释。KIBRA(肾脑表达蛋白)和CLSTN2(钙结合蛋白2)是先前与情景记忆表现及海马体(关键记忆结构)体积相关的两个候选基因。然而,这两个基因的多态性是否也影响与年龄相关的纵向记忆衰退和海马萎缩仍不清楚。利用来自悉尼记忆与衰老研究和澳大利亚老年双胞胎研究这两个独立队列的数据,我们调查了KIBRA和CLSTN2基因多态性(rs17070145和rs6439886)是否与老年人(基线年龄65 - 90岁)的情景记忆表现和海马体积相关。我们能够使用横断面数据,更重要的是,还使用纵向数据(两次测试间隔2年)来研究这些多态性与记忆和海马体积的关系。总体而言,我们没有发现单独的KIBRA或与CLSTN2联合起来与记忆表现或海马体积存在关联的证据,这些基因的变异也未影响两个老年人群队列中的纵向记忆衰退或海马萎缩。

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