脑衰老和阿尔茨海默病中突触外GluN2B受体亚基和多唾液酸神经细胞黏附分子的时空差异调节
Spatiotemporal differential regulation of extrasynaptic GluN2B receptor subunits and PSA-NCAM in brain aging and Alzheimer's disease.
作者信息
Imiruaye Oghenetega E, Perez Isis G, Carson Brian C, Crouzet Christian, Garcia Jerome, Han Derick, Bhattacharya Subhrajit
机构信息
Henry E. Riggs School of Applied Life Sciences, Keck Graduate Institute, Claremont, CA, United States.
Beckman Laser Institute and Medical Clinic, University of California, Irvine, Irvine, CA, United States.
出版信息
Front Neurosci. 2025 Aug 29;19:1649625. doi: 10.3389/fnins.2025.1649625. eCollection 2025.
INTRODUCTION
Extrasynaptic GluN2B N-methyl-D-aspartate receptors (ES-GluN2B) are localized outside synapses and promote excitotoxic signaling, apoptosis, and long-term depression (LTD) in Alzheimer's disease (AD). Polysialylated neural cell adhesion molecule (PSA-NCAM) physiologically inhibits ES-GluN2B activity, and its downregulation is associated with impaired synaptic plasticity. However, the spatiotemporal changes of ES-GluN2B and PSA-NCAM during brain aging versus AD remain poorly understood.
METHODS
We investigated GluN2A, GluN2B, ES-GluN2B, and PSA-NCAM expression across brain regions in young and old Tg2576 AD and wild-type (WT) mice. Additional experiments included PSD-95 pulldown assays, analysis of GluN2B phosphorylation at Ser1480, CRISPRa-driven ST8Sia4 upregulation in IMR-32 neuroblastoma cells, and Aβ treatment to assess effects on PSA-NCAM biosynthetic enzymes.
RESULTS
Normal aging was associated with decreased GluN2B, increased GluN2A, stable ES-GluN2B, and elevated PSA-NCAM levels. In contrast, AD aging showed elevated ES-GluN2B and reduced PSA-NCAM, particularly in the hippocampus and cortex, with no change in total NCAM expression. PSD-95 pulldown revealed increased extrasynaptic GluN2B in aged AD brains. AD aging was associated with elevated phosphorylation of GluN2B at Ser1480 by casein kinase 2 (CK2), promoting GluN2B redistribution to extrasynaptic sites. CRISPRa-driven ST8Sia4 upregulation increased PSA-NCAM and reduced pGluN2B expression supporting a direct regulatory role for PSA-NCAM in GluN2B trafficking. Additionally, Aβ suppressed PSA-NCAM biosynthetic enzymes ST8Sia4 and UDP-E linking Aβ to impaired polysialylation.
DISCUSSION
These findings highlight distinct regulatory patterns of ES-GluN2B and PSA-NCAM in AD versus normal aging and support a model in which impaired PSA-NCAM buffering facilitates pathological ES-GluN2B signaling and plasticity loss in AD progression.
引言
突触外N-甲基-D-天冬氨酸受体2B(ES-GluN2B)定位于突触之外,在阿尔茨海默病(AD)中促进兴奋性毒性信号传导、细胞凋亡和长时程抑制(LTD)。多唾液酸神经细胞粘附分子(PSA-NCAM)在生理上抑制ES-GluN2B的活性,其下调与突触可塑性受损有关。然而,在大脑衰老与AD过程中ES-GluN2B和PSA-NCAM的时空变化仍知之甚少。
方法
我们研究了年轻和年老的Tg2576 AD小鼠及野生型(WT)小鼠大脑各区域中GluN2A、GluN2B、ES-GluN2B和PSA-NCAM的表达。额外的实验包括PSD-95下拉实验、对Ser1480位点GluN2B磷酸化的分析、在IMR-32神经母细胞瘤细胞中通过CRISPRa驱动ST8Sia4上调以及Aβ处理以评估对PSA-NCAM生物合成酶的影响。
结果
正常衰老与GluN2B减少、GluN2A增加、ES-GluN2B稳定以及PSA-NCAM水平升高有关。相比之下,AD相关衰老表现为ES-GluN2B升高和PSA-NCAM减少,特别是在海马体和皮质,总NCAM表达无变化。PSD-95下拉实验显示老年AD大脑中突触外GluN2B增加。AD相关衰老与酪蛋白激酶2(CK2)导致的Ser1480位点GluN2B磷酸化升高有关,促进GluN2B重新分布到突触外位点。CRISPRa驱动的ST8Sia4上调增加了PSA-NCAM并降低了pGluN2B表达,支持PSA-NCAM在GluN2B转运中起直接调节作用。此外,Aβ抑制了PSA-NCAM生物合成酶ST8Sia4和UDP-E,将Aβ与多唾液酸化受损联系起来。
讨论
这些发现突出了AD与正常衰老过程中ES-GluN2B和PSA-NCAM不同的调节模式,并支持一种模型,即PSA-NCAM缓冲功能受损促进了AD进展过程中病理性ES-GluN2B信号传导和可塑性丧失。
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