Abstract
Astrocytes serve essential roles in human brain function and diseases. Growing evidence indicates that astrocytes are central players of the feedback modulation of excitatory Glu signalling during epileptiform activity via Glu-GABA exchange. The underlying mechanism results in the increase of tonic inhibition by reverse operation of the astroglial GABA transporter, induced by Glu-Na+ symport. GABA, released from astrocytes, is synthesized from the polyamine (PA) putrescine and this process involves copper amino oxidase. Through this pathway, putrescine can be considered as an important source of inhibitory signaling that counterbalances epileptic discharges. Putrescine, however, is also a precursor for spermine that is known to enhance gap junction channel communication and, consequently, supports long-range Ca2+ signaling and contributes to spreading of excitatory activity through the astrocytic syncytium. Recently, we presented the possibility of neuron-glia redox coupling through copper (Cu+/Cu2+) signaling and oxidative putrescine catabolism. In the current work, we explore whether the Cu+/Cu2+ homeostasis is involved in astrocytic control on neuronal excitability by regulating PA catabolism. We provide supporting experimental data underlying this hypothesis. We show that the blockade of copper transporter (CTR1) by AgNO3 (3.6 µM) prevents GABA transporter-mediated tonic inhibitory currents, indicating causal relationship between copper (Cu+/Cu2+) uptake and the catabolism of putrescine to GABA in astrocytes. In addition, we show that MnCl2 (20 μM), an inhibitor of the divalent metal transporter DMT1, also prevents the astrocytic Glu-GABA exchange. Furthermore, we observed that facilitation of copper uptake by added CuCl2 (2 µM) boosts tonic inhibitory currents. These findings corroborate the hypothesis that modulation of neuron-glia coupling by copper uptake drives putrescine → GABA transformation, which leads to subsequent Glu-GABA exchange and tonic inhibition. Findings may in turn highlight the potential role of copper signaling in fine-tuning the activity of the tripartite synapse.
Highlights
In order to assess the potential role for CTR1 in putrescine metabolism and GluGABA exchange, here we explored whether inhibition of CTR1 by Ag+ [45] or inhibition of the divalent metal transporter DMT1 by Mn2+ [46] affect the Glu-GABA exchangecontrolled tonic inhibition in rat hippocampal slices
To explore whether copper uptake plays a role in putrescine-dependent tonic inhibition provided by astrocytes [25,26], we measured inhibitory currents on hippocampal
We investigated the relationship between copper uptake, PA metabolism and subsequent astrocytic regulation of neuronal excitability
Summary
Beside neuronal activitydependent astroglial energy metabolisms [9], neuron-glia coupling may involve K+ , Ca2+. Na+ signalling through gap junction channels (GJCs), astroglial Glu-Na+ symportevoked release of GABA (Glu-GABA exchange), glycine, glutamine and other neuro/glio transmitters or modulators [10,11,12,13,14,15,16,17,18,19,20,21,22,23,24]. Astroglial GABA release mechanisms involve inside-out (reverse) operation of astroglial GABA transporters GAT-2/3 [15,25,26] or bestrophin 1 channels [27,28,29]. GABA may travel far away from the tripartite synapse through astrocytic Cx43 GJCs, facilitated by polyamines (PAs) [30,31]. 4.0/).
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