Volume transmission signalling via astrocytes

Hirase, Hajime; Iwai, Yoshio; Takata, Norio; Shinohara, Yuta; Mishima, Tatsuya

doi:10.1098/rstb.2013.0604

Cited by 50 publications

(37 citation statements)

References 91 publications

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“…What signals-neuronal or nonneuronal, intra-or extracellular, synchronized or desynchronized-cause the intracellular astrocytic Ca 2+ rises that occur before the state switch? There has been recent focus on mechanisms of focal Ca 2+ activation in astrocyte processes, both synaptic and nonsynaptic (30,33,34,47,62), but no broad consensus yet exists. G protein-coupled receptor (GPCR) activation and release of Ca 2+ from intercellular stores via IP 3 receptors is an accepted pathway for Ca 2+ increases in astrocyte somata (63,64), although it has recently been argued that this mechanism may not explain Ca 2+ increases in astrocyte processes (30).…”

Section: Discussionmentioning

confidence: 99%

Astrocytes regulate cortical state switching in vivo

Poskanzer

Yuste

2016

Proc. Natl. Acad. Sci. U.S.A.

333

304

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The role of astrocytes in neuronal function has received increasing recognition, but disagreement remains about their function at the circuit level. Here we use in vivo two-photon calcium imaging of neocortical astrocytes while monitoring the activity state of the local neuronal circuit electrophysiologically and optically. We find that astrocytic calcium activity precedes spontaneous circuit shifts to the slow-oscillation-dominated state, a neocortical rhythm characterized by synchronized neuronal firing and important for sleep and memory. Further, we show that optogenetic activation of astrocytes switches the local neuronal circuit to this slow-oscillation state. Finally, using two-photon imaging of extracellular glutamate, we find that astrocytic transients in glutamate co-occur with shifts to the synchronized state and that optogenetically activated astrocytes can generate these glutamate transients. We conclude that astrocytes can indeed trigger the low-frequency state of a cortical circuit by altering extracellular glutamate, and therefore play a causal role in the control of cortical synchronizations.he neocortical slow oscillation (∼1 Hz) that defines slowwave sleep (SWS) is believed to play a critical role in memory consolidation by coordinating cell assemblies in areas within and outside the cortex (1-4). This cortical state is in marked contrast to rapid-eye-movement (REM) sleep and wakefulness, which are dominated by low-amplitude and high-frequency cortical activity (5). Slow cortical rhythms are also observed during the waking state, as well as during sleep (6-10), suggesting widespread functional roles for this oscillation. Although the slow oscillation is cortically generated (11)(12)(13)(14), the circuit mechanisms that drive the cortex into the slow-wave state remain unclear. Because neuronal responses to external stimuli are modulated by brain state, the mechanisms that drive transitions to different states-the relatively synchronized, slow-oscillation-dominated state or the desynchronized, more "awake" or attentive state-have recently been of intense interest, although most of these have focused on the shift to the desynchronized state (15)(16)(17)(18)(19). These studies have critically examined the effects of neuronal and sensory manipulations on brain state and the effects of brain state on processing, but have not investigated how other cellular circuit components may influence these states.Astrocytes have been implicated in SWS and the regulation of UP states-the cellular underpinnings of the slow oscillation (20-23)-and are attractive candidates for carrying out a widespread circuit role because each astrocyte has the potential to influence thousands of synapses simultaneously (24). However, the methodology used to demonstrate an astrocyte-specific function in regulation of SWS (21) and the slow oscillation (22) has become controversial (25, 26), leaving astrocytes' role in the generation of the slow-oscillation state uncertain. In addition, there are few data on astrocytes' roles in acu...

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Section: Discussionmentioning

confidence: 99%

Astrocytes regulate cortical state switching in vivo

Poskanzer

Yuste

2016

Proc. Natl. Acad. Sci. U.S.A.

333

304

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“…Interestingly, neuromodulator signalling often relies on volume transmission that sets a long-range and long-lasting tone of neuromodulator, affecting many targets over prolonged periods of time [75]. The fact that astrocytes respond to neuromodulators therefore further illustrates how their action on synapses is mostly geared towards slower and more durable tuning of synaptic properties.…”

Section: (C) Astrocytes Sense Neuromodulatorsmentioning

confidence: 99%

Astrocytic control of synaptic function

Papouin

Dunphy

Tolman

et al. 2017

Phil. Trans. R. Soc. B

204

137

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One contribution of 16 to a discussion meeting issue 'Integrating Hebbian and homeostatic plasticity'. Astrocytes intimately interact with synapses, both morphologically and, as evidenced in the past 20 years, at the functional level. Ultrathin astrocytic processes contact and sometimes enwrap the synaptic elements, sense synaptic transmission and shape or alter the synaptic signal by releasing signalling molecules. Yet, the consequences of such interactions in terms of information processing in the brain remain very elusive. This is largely due to two major constraints: (i) the exquisitely complex, dynamic and ultrathin nature of distal astrocytic processes that renders their investigation highly challenging and (ii) our lack of understanding of how information is encoded by local and global fluctuations of intracellular calcium concentrations in astrocytes. Here, we will review the existing anatomical and functional evidence of local interactions between astrocytes and synapses, and how it underlies a role for astrocytes in the computation of synaptic information.This article is part of the themed issue 'Integrating Hebbian and homeostatic plasticity'.

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“…In these regions, the ACh tone fluctuates with changes in vigilance state: the highest levels are found during active wakefulness and the lowest during slow wave sleep (Marrosu et al, 1995; Lee et al, 2005; Zant et al, 2016). Interestingly, ACh is known to influence NMDAR activity and NMDAR-dependent functions (Kirkwood et al, 1999; Lin et al, 2013; Markram and Segal, 1990; Yang et al, 2013; Zappettini et al, 2014), and activates intracellular signaling in astrocytes through various ACh receptors (AChRs) (Hirase et al, 2014; Sharma and Vijayaraghavan, 2001; Shen and Yakel, 2012; Takata et al, 2011). Combined with evidence that ACh can promote D-serine synthesis and/or release (Lin et al, 2013; Singh et al, 2013; Takata et al, 2011), these data point to a link between vigilance state-dependent cholinergic activity and NMDAR co-agonist gating via astrocytic D-serine.…”

Section: Introductionmentioning

confidence: 99%

“…This makes astrocytes good candidates to receive, integrate and relay information about the neuromodulatory state of the brain, such that their impact on neuronal and brain function has become increasingly relevant in the scope of behavioral states (Chen et al, 2012; Ding et al, 2013; Hirase et al, 2014; Panatier at al., 2006; Schmitt et al, 2012; Paukert et al, 2014). This is supported by evidence that astrocytes are exquisite sensors of neuromodulators, such as norepinephrine and acetylcholine, that are involved in sensory modalities and vigilance states (Ding et al, 2013; Lee et al, 2005; Paukert et al, 2014; Pinto et al, 2013; Hirase et al, 2014; Navarrete et al, 2012; Sharma and Vijayaraghavan, 2001; Shen and Yakel, 2012; Takata et al, 2011). Here we used a variety of in vivo and in vitro approaches to examine fluctuations of endogenous D-serine availability throughout the day and their link with cholinergic activity.…”

Section: Introductionmentioning

confidence: 99%

Septal Cholinergic Neuromodulation Tunes the Astrocyte-Dependent Gating of Hippocampal NMDA Receptors to Wakefulness

Papouin

Dunphy

Tolman

et al. 2017

Neuron

205

222

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Summary The activation of the N-methyl D-aspartate receptor (NMDAR) is controlled by a glutamate-binding site and a distinct, independently regulated, co-agonist-binding site. In most brain regions, the NMDAR co-agonist is the astrocyte-derived gliotransmitter D-serine. We found that D-serine levels oscillate in mouse hippocampus as a function of wakefulness, in vitro and in vivo. This causes a full saturation of the NMDAR co-agonist site in the dark (active)-phase that dissipates to sub-saturating levels during the light (sleep)-phase, and influences learning performance throughout the day. We demonstrate that hippocampal astrocytes sense the wakefulness-dependent activity of septal cholinergic fibers through the α7-nicotinic acetylcholine receptor (α7nAChR), whose activation drives D-serine release. We conclude that astrocytes tune the gating of synaptic NMDARs to the vigilance state and demonstrate that this is directly relevant to schizophrenia, a disorder characterized by NMDAR and cholinergic hypofunctions. Indeed, bypassing cholinergic activity with a clinically-tested α7nAChR agonist successfully enhances NMDARs activation.

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Volume transmission signalling via astrocytes

Cited by 50 publications

References 91 publications

Astrocytes regulate cortical state switching in vivo

Astrocytes regulate cortical state switching in vivo

Astrocytic control of synaptic function

Septal Cholinergic Neuromodulation Tunes the Astrocyte-Dependent Gating of Hippocampal NMDA Receptors to Wakefulness

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