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首页> 外文期刊>Scientific reports. >KIBRA is associated with accelerated cognitive decline and hippocampal atrophy in APOE ε4-positive cognitively normal adults with high Aβ-amyloid burden
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KIBRA is associated with accelerated cognitive decline and hippocampal atrophy in APOE ε4-positive cognitively normal adults with high Aβ-amyloid burden

机译:Kibra与Apoeε4阳性认知正常成虫的加速认知下降和海马萎缩有关,具有高Aβ-淀粉样料

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摘要

A single nucleotide polymorphism, rs17070145, in the KIdney and BRAin expressed protein (KIBRA) gene has been associated with cognition and hippocampal volume in cognitively normal (CN) individuals. However, the impact of rs17070145 on longitudinal cognitive decline and hippocampal atrophy in CN adults at greatest risk of developing Alzheimer’s disease is unknown. We investigated the impact rs17070145 has on the rate of cognitive decline and hippocampal atrophy over six years in 602 CN adults, with known brain Aβ-amyloid levels and whether there is an interactive effect with APOE genotype. We reveal that whilst limited independent effects of KIBRA genotype were observed, there was an interaction with APOE in CN adults who presented with high Aβ-amyloid levels across study duration. In comparison to APOE ε4-ve individuals carrying the rs17070145-T allele, significantly faster rates of cognitive decline (global, p?=?0.006; verbal episodic memory, p?=?0.004), and hippocampal atrophy (p?=?0.04) were observed in individuals who were APOE ε4?+?ve and did not carry the rs17070145-T allele. The observation of APOE effects in only non-carriers of the rs17070145-T allele, in the presence of high Aβ-amyloid suggest that carriers of the rs17070145-T allele are conferred a level of resilience to the detrimental effects of high Aβ-amyloid and APOE ε4.
机译:单个核苷酸多态性,RS17070145,肾脏和脑表达蛋白(KIBRA)基因已经与认知正常(CN)个体中的认知和海马体积相关。然而,RS17070145对CN成年人的纵向认知下降和海马萎缩的影响,以最大的发展Alzheimer疾病的风险是未知的。我们调查了RS17070145的影响,在602 CN成年人中有超过六年的认知下降和海马萎缩的影响,具有已知的脑Aβ-淀粉样蛋白水平,以及是否存在与ApoE基因型的交互式效果。我们揭示了观察到kibra基因型的有限的独立效果,而在研究持续时间呈现高β-淀粉样液水平的CN成年人中的相互作用。与携带RS17070145-T等位基因的Apoeε4-ve,认知下降的速度明显更快(全球性,P?= 0.006;口头集诊记忆,p?= 0.004)和海马萎缩(p?= 0.04在Apoeε4的个体中观察到的是ε4?+ ve并且没有携带RS17070145-T等位基因。在高Aβ-淀粉样蛋白的存在下,仅在RS17070145-T等位基因的存在下观察APOE效应,表明RS17070145-T等位基因的载体赋予高Aβ-淀粉样蛋白和高Aβ-淀粉样蛋白的有害影响apoeε4。

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