长期苯二氮䓬治疗诱导的NMDAR活性增加和GluN2A-NMDAR沉默突触扩展。
Increased NMDAR activity and GluN2A-NMDAR silent synapse expansion induced by chronic benzodiazepine treatment.
作者信息
Chapman Caitlyn A, Povysheva Nadya, Johnson Jon W, Jacob Tija C
机构信息
Department of Pharmacology and Chemical Biology, University of Pittsburgh School of Medicine, Pittsburgh, PA, USA.
Department of Neuroscience and Center for Neuroscience, University of Pittsburgh, Pittsburgh, PA, USA.
出版信息
Neuropharmacology. 2025 Nov 15;279:110624. doi: 10.1016/j.neuropharm.2025.110624. Epub 2025 Aug 5.
Benzodiazepines (BZDs) are critical sedative, anticonvulsant, and anxiolytic drugs that potentiate inhibitory GABAergic neurotransmission. However, clinical utility is hampered by drug tolerance and a hyperexcitable withdrawal syndrome characterized by neuronal excitation/inhibition (E/I) imbalance. Although enhanced excitation is implicated in BZD tolerance, the homeostatic changes to glutamatergic receptors remain undefined. Here, we report the impact of chronic (7-day) BZD treatment on excitatory synapse and NMDA receptor (NMDAR) function, expression, and subcellular localization in cortical neurons. Chronic treatment with the BZD diazepam (DZP) resulted in an increase in NMDAR-mediated miniature excitatory postsynaptic currents (mEPSCs). Confocal imaging studies revealed a DZP-induced enrichment of GluN2B-containing NMDARs at functional synapses (expressing AMPA receptors, AMPARs) while GluN2B subunit expression was otherwise unaltered. Conversely, localization of GluN2A-containing NMDARs (GluN2A-NMDARs) to functional synapses was unchanged, while GluN2A-NMDAR total protein levels and surface accumulation were enhanced. Intriguingly, we demonstrate for the first time the BZD-induced enrichment and expansion of GluN2A-NMDAR coverage at silent (AMPAR-lacking) synapses. Finally, biochemical fractionation analysis of the translation elongation protein eEF2, known to control E/I balance, detected lower levels of deactivated, phosphorylated eEF2 in the synaptic fraction of DZP-treated neurons, indicative of enhanced local translation. Collectively, our findings suggest that chronic BZD treatment triggers compensatory mechanisms which 1) enhance NMDAR function via increased GluN2B-NMDARs at functional synapses, and 2) promote the expression, surface localization, and accumulation of GluN2A-NMDARs at silent synapses, augmenting the potential for further synaptic plasticity.
苯二氮䓬类药物(BZDs)是重要的镇静、抗惊厥和抗焦虑药物,可增强抑制性γ-氨基丁酸(GABA)能神经传递。然而,药物耐受性和以神经元兴奋/抑制(E/I)失衡为特征的过度兴奋戒断综合征妨碍了其临床应用。尽管增强的兴奋与BZD耐受性有关,但谷氨酸能受体的稳态变化仍不明确。在此,我们报告了慢性(7天)BZD治疗对皮质神经元兴奋性突触和N-甲基-D-天冬氨酸受体(NMDAR)功能、表达及亚细胞定位的影响。用BZD地西泮(DZP)进行慢性治疗导致NMDAR介导的微小兴奋性突触后电流(mEPSCs)增加。共聚焦成像研究显示,DZP诱导含GluN2B的NMDAR在功能性突触(表达α-氨基-3-羟基-5-甲基-4-异恶唑丙酸受体,AMPARs)处富集,而GluN2B亚基的表达未发生改变。相反,含GluN2A的NMDAR(GluN2A-NMDARs)在功能性突触处的定位未变,而GluN2A-NMDAR的总蛋白水平和表面聚集增加。有趣的是,我们首次证明了BZD诱导GluN2A-NMDAR在沉默(缺乏AMPAR)突触处的富集和覆盖范围扩大。最后,对已知可控制E/I平衡的翻译延伸蛋白eEF2进行的生化分级分离分析发现,DZP处理神经元的突触部分中失活的、磷酸化的eEF2水平较低,表明局部翻译增强。总的来说,我们的研究结果表明,慢性BZD治疗触发了补偿机制,1)通过在功能性突触处增加含GluN2B的NMDAR来增强NMDAR功能,2)促进GluN2A-NMDAR在沉默突触处的表达、表面定位和聚集,增加进一步突触可塑性的潜力。
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