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阿尔茨海默病中的表观遗传改变:DNA 甲基化减少。

Epigenetic changes in Alzheimer's disease: decrements in DNA methylation.

机构信息

L.J. Roberts Center for Alzheimer's Research, Sun Health Research Institute, P.O. Box 1278, Sun City, AZ 85372, USA.

出版信息

Neurobiol Aging. 2010 Dec;31(12):2025-37. doi: 10.1016/j.neurobiolaging.2008.12.005. Epub 2008 Dec 30.

Abstract

DNA methylation is a vital component of the epigenetic machinery that orchestrates changes in multiple genes and helps regulate gene expression in all known vertebrates. We evaluated immunoreactivity for two markers of DNA methylation and eight methylation maintenance factors in entorhinal cortex layer II, a region exhibiting substantial Alzheimer's disease (AD) pathology in which expression changes have been reported for a wide variety of genes. We show, for the first time, neuronal immunoreactivity for all 10 of the epigenetic markers and factors, with highly significant decrements in AD cases. These decrements were particularly marked in PHF1/PS396 immunoreactive, neurofibrillary tangle-bearing neurons. In addition, two of the DNA methylation maintenance factors, DNMT1 and MBD2, have been reported also to interact with ribosomal RNAs and ribosome synthesis. Consistent with these findings, DNMT1 and MBD2, as well as p66α, exhibited punctate cytoplasmic immunoreactivity that co-localized with the ribosome markers RPL26 and 5.8s rRNA in ND neurons. By contrast, AD neurons generally lacked such staining, and there was a qualitative decrease in RPL26 and 5.8s rRNA immunoreactivity. Collectively, these findings suggest epigenetic dysfunction in AD-vulnerable neurons.

摘要

DNA 甲基化是表观遗传机制的重要组成部分,它协调多个基因的变化,并帮助调节所有已知脊椎动物的基因表达。我们评估了二种 DNA 甲基化标志物和八种甲基化维持因子在海马回皮质 II 层中的免疫反应性,该区域在阿尔茨海默病(AD)病理中表现出大量的变化,其中已报道了广泛的基因表达变化。我们首次展示了所有 10 种表观遗传标志物和因子的神经元免疫反应性,AD 病例中的这些标志物和因子的免疫反应性显著降低。在 PHF1/PS396 免疫反应阳性的神经原纤维缠结携带神经元中,这种降低尤为明显。此外,两种 DNA 甲基化维持因子,DNMT1 和 MBD2,也被报道与核糖体 RNA 和核糖体合成相互作用。与这些发现一致的是,DNMT1 和 MBD2 以及 p66α 表现出点状细胞质免疫反应性,与 ND 神经元中的核糖体标记物 RPL26 和 5.8s rRNA 共定位。相比之下,AD 神经元通常缺乏这种染色,并且 RPL26 和 5.8s rRNA 免疫反应性也存在定性降低。总之,这些发现表明 AD 易感神经元中存在表观遗传功能障碍。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/b0f0/2962691/61a9e581004c/nihms-244885-f0001.jpg

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