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淀粉样前体蛋白突变破坏了阿尔茨海默病小鼠模型中生殖经验增强的正常认知发展。

Amyloid precursor protein mutation disrupts reproductive experience-enhanced normal cognitive development in a mouse model of Alzheimer's disease.

作者信息

Cui Jie, Jothishankar Balaji, He Ping, Staufenbiel Matthias, Shen Yong, Li Rena

机构信息

Center for Hormone Advanced Science and Education, Roskamp Institute, 2040 Whitfield Avenue, Sarasota, FL, 34243, USA.

出版信息

Mol Neurobiol. 2014 Feb;49(1):103-12. doi: 10.1007/s12035-013-8503-x. Epub 2013 Jul 14.

Abstract

Women experience dramatic changes in hormones, mood and cognition through different periods of their reproductive lives, particularly during pregnancy and giving birth. While limited human studies of early pregnancy and motherhood showed alteration of cognitive functions in later life, researches on rodents showed a persistent improvement of learning and memory performance in females with history of giving birth compared to virgin controls. Alzheimer's disease (AD), the most common dementia in elderly, is more prevalent in women than in men. One of the risk factors is related to the sharp reduction of estrogen in aged women. It is unknown whether the history of fertility activity plays any roles in altering risk of AD in females, such as altering cognitive function. Would reproductive experience alter the risk of AD in females? If so, what might be the mechanisms of the change? In this study, we examined the effects of reproductive experience on cognitive function in an AD transgenic mouse model (APP23) and age-matched wild-type non-transgenic control mice (WT). Our data showed an age-dependent effect of reproductive experience on learning and memory activity between breeders (had one or more litters) and non-breeders (virgins). More importantly, our data, for the first time, demonstrated a genotype-dependent effect of parity on cognitive function between APP23 and WT mice. At the age of 12 months, WT breeders outperform non-breeders in spatial working and reference memory while APP23 breeders performed worse in spatial learning and memory than age-matched APP23 non-breeders. These genotype- and age-dependent effects of reproductive activity on cognitions are significantly associated with changes of neuropathology of AD in the APP23 mice, expression of proteins related to synaptic plasticity and cognitive functions in the brain.

摘要

在整个生殖生命过程中,女性的激素、情绪和认知会经历巨大变化,尤其是在怀孕和分娩期间。虽然关于早期妊娠和为人母的人体研究有限,显示晚年认知功能会发生改变,但对啮齿动物的研究表明,与未生育的对照组相比,有生育史的雌性动物的学习和记忆能力持续改善。阿尔茨海默病(AD)是老年人中最常见的痴呆症,女性比男性更普遍。其中一个风险因素与老年女性雌激素的急剧减少有关。尚不清楚生育活动史是否在改变女性患AD的风险方面发挥任何作用,比如改变认知功能。生殖经历会改变女性患AD的风险吗?如果是这样,这种变化的机制可能是什么?在本研究中,我们在AD转基因小鼠模型(APP23)和年龄匹配的野生型非转基因对照小鼠(WT)中研究了生殖经历对认知功能的影响。我们的数据显示,繁殖者(有一窝或多窝幼崽)和非繁殖者(未生育)之间,生殖经历对学习和记忆活动存在年龄依赖性影响。更重要的是,我们的数据首次证明了产次对APP23和WT小鼠认知功能的基因型依赖性影响。在12个月大时,WT繁殖者在空间工作记忆和参考记忆方面优于非繁殖者,而APP23繁殖者在空间学习和记忆方面比年龄匹配的APP23非繁殖者表现更差。生殖活动对认知的这些基因型和年龄依赖性影响与APP23小鼠AD神经病理学的变化、大脑中与突触可塑性和认知功能相关的蛋白质表达显著相关。

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