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阿尔茨海默病中与年龄相关的基因表达变化加速。

Age-related changes in gene expression are accelerated in Alzheimer's disease.

机构信息

Department of Clinical Neuroscience, Karolinska Institute and Hospital, R5:00, SE-171 76 Stockholm, Sweden.

出版信息

Synapse. 2011 Sep;65(9):971-4. doi: 10.1002/syn.20933. Epub 2011 Apr 11.

Abstract

In the normal brain, age is associated with changes in gene expression. Age is also a prominent risk factor for Alzheimer's disease (AD), where clinical features are similar to age-related decreases in cognitive performance. We hypothesized that some age-related changes in gene expression are accelerated in AD patients. To study this, we selected 10 candidate genes earlier shown by microarray analysis to be differentially expressed in AD (Emilsson et al., [2006] Neurobiol Dis 21:618-625). Using real-time PCR analysis and a control based statistical model, we investigated age-related changes in mRNA levels in a large collection of human brain postmortem tissues from AD patients and controls. Our results demonstrate that the age-related changes in gene expression are manifested earlier in AD. Furthermore, five of the genes (ITPKB, RGS4, RAB3A, STMN1, SYNGR3) have in common an involvement in neuronal calcium dependent signaling, a cellular process previously related to both AD and aging. These observations suggest that coordinated transcriptional changes associated with ageing and calcium homeostasis in the human brain are accelerated in patients with AD. Our results point to the possibility that the activity of these genes can be used in the future as a palette of biomarkers for predicting disease risk in young individuals.

摘要

在正常的大脑中,年龄与基因表达的变化有关。年龄也是阿尔茨海默病(AD)的一个突出风险因素,其临床特征与认知表现随年龄增长而下降相似。我们假设 AD 患者的某些与年龄相关的基因表达变化会加速。为了研究这一点,我们选择了 10 个候选基因,这些基因之前通过微阵列分析显示在 AD 中表达差异(Emilsson 等人,[2006]Neurobiol Dis 21:618-625)。使用实时 PCR 分析和基于对照的统计模型,我们研究了来自 AD 患者和对照的大量人脑尸检组织中 mRNA 水平的与年龄相关的变化。我们的结果表明,AD 患者的基因表达与年龄相关的变化更早出现。此外,其中五个基因(ITPKB、RGS4、RAB3A、STMN1、SYNGR3)共同参与神经元钙依赖性信号转导,这是一个先前与 AD 和衰老都有关的细胞过程。这些观察结果表明,与衰老和人类大脑钙稳态相关的协调转录变化在 AD 患者中加速。我们的结果表明,这些基因的活性将来可能被用作预测年轻人患病风险的生物标志物。

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