Polyamines have fundamental roles in brain homeostasis as key modulators of cellular excitability. Several studies have suggested alterations in polyamine metabolism in stress related disorders, suicide, depression, and neurodegeneration, making the pharmacological modulation of polyamines a highly appealing therapeutic strategy. Polyamines are small aliphatic molecules that can modulate cationic channels involved in neuronal excitability. Previous indirect evidence has suggested that polyamines can modulate anionic GABAA receptors (GABAARs), which mediate inhibitory signaling and provide a direct route to reduce hyperexcitability. Here, we attempted to characterize the effect that spermine, the polyamine with the strongest reported effect on GABAARs, has on human postmortem native GABAARs. We microtransplanted human synaptic membranes from the dorsolateral prefrontal cortex of four cases with no history of mental or neurological disorders, and directly recorded spermine effects on ionic GABAARs responses on microtransplanted oocytes. We show that in human synapses, inhibition of GABAARs by spermine was better explained by alkalization of the extracellular solution. Additionally, spermine had no effect on the potentiation of GABA-currents by diazepam, indicating that even if diazepam binding is enhanced by spermine, it does not translate to changes in functional activity. Our results clearly demonstrate that while extracellular spermine does not have direct effects on human native synaptic GABAARs, spermine-mediated shifts of pH inhibit GABAARs. Potential spermine-mediated increase of pH in synapses in vivo may therefore participate in increased neuronal activity observed during physiological and pathological states, and during metabolic alterations that increase the release of spermine to the extracellular milieu.

译文

:多胺作为细胞兴奋性的关键调节剂,在脑稳态中具有基本作用。多项研究表明,与应激有关的疾病,自杀,抑郁和神经退行性疾病中多胺代谢的改变,使多胺的药理学调节成为极具吸引力的治疗策略。多胺是小的脂肪族分子,可以调节神经元兴奋性所涉及的阳离子通道。先前的间接证据表明,多胺可调节阴离子性GABAA受体(GABAARs),介导抑制性信号传导并提供降低过度兴奋性的直接途径。在这里,我们试图表征精胺(对GABAARs报道作用最强的多胺)对人类尸体天然GABAARs的影响。我们从4例无精神或神经疾病病史的背外侧前额叶皮层微移植了人类突触膜,并直接记录了精胺对微移植卵母细胞离子GABAARs反应的影响。我们显示,在人类突触中,精胺对GABAAR的抑制作用可以通过细胞外溶液的碱化得到更好的解释。另外,精胺对地西epa对GABA电流的增强没有影响,表明即使精胺增强了地西epa的结合,它也不会转化为功能活性的改变。我们的结果清楚地表明,虽然细胞外精胺对人类天然突触GABAAR没有直接影响,但精胺介导的pH改变会抑制GABAAR。因此,潜在的精胺介导的体内突触中pH值的增加可能参与了生理和病理状态以及代谢改变(增加了精胺向细胞外环境的释放)过程中观察到的神经元活性的增加。

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