Journal
NEURON
Volume 68, Issue 1, Pages 113-126Publisher
CELL PRESS
DOI: 10.1016/j.neuron.2010.08.043
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Funding
- Ministerio de Genoa e Innovacion, Spain [8FU2007-064764]
- European Union [HEALTH-F2-2007-202167]
- Cajal Blue Brain
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Endocannabinoids and their receptor CB1 play key roles in brain function. Astrocytes express CB1 Rs that are activated by endocannabinoids released by neurons. However, the consequences of the endocannabinoid-mediated neuron-astrocyte signaling on synaptic transmission are unknown. We show that endocannabinoids released by hippocampal pyramidal neurons increase the probability of transmitter release at CA3-CA1 synapses. This synaptic potentiation is due to CB1R-induced Ca2+ elevations in astrocytes, which stimulate the release of glutamate that activates presynaptic metabotropic glutamate receptors. While endocannabinoids induce synaptic depression in the stimulated neuron by direct activation of presynaptic CB1 Rs, they indirectly lead to synaptic potentiation in relatively more distant neurons by activation of CB1 Rs in astrocytes. Hence, astrocyte calcium signal evoked by endogenous stimuli (neuron-released endocannabinoids) modulates synaptic transmission. Therefore, astrocytes respond to endocannabinoids that then potentiate synaptic transmission, indicating that astrocytes are actively involved in brain physiology.
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