Specialized astrocytes mediate glutamatergic gliotransmission in the CNS

Roberta De Ceglia(University of Lausanne), Ada Ledonne(Fondazione Santa Lucia), David Litvin(Wyss Center for Bio and Neuroengineering), Barbara Lykke Lind(University of Copenhagen), Giovanni Carriero(University of Lausanne), Emanuele Claudio Latagliata(Fondazione Santa Lucia), Erika Bindocci(University of Lausanne), Maria Amalia Di Castro(Sapienza University of Rome), Iaroslav Savtchouk(Marquette University), Ilaria Vitali(University of Lausanne), Anurag Ranjak(University of Lausanne), Mauro Congiu(University of Lausanne), Tara Canonica(University of Lausanne), William Wisden(UK Dementia Research Institute), Kenneth D. Harris(National Hospital for Neurology and Neurosurgery), Manuel Mameli(University of Lausanne), Nicola Biagio Mercuri(University of Rome Tor Vergata), Ludovic Telley(University of Lausanne), Andrea Volterra(Wyss Center for Bio and Neuroengineering)
Nature
September 6, 2023
10.1038/s41586-023-06502-w
Cited by 263Open Access
Full Text

Abstract

Abstract Multimodal astrocyte–neuron communications govern brain circuitry assembly and function 1 . For example, through rapid glutamate release, astrocytes can control excitability, plasticity and synchronous activity 2,3 of synaptic networks, while also contributing to their dysregulation in neuropsychiatric conditions 4–7 . For astrocytes to communicate through fast focal glutamate release, they should possess an apparatus for Ca 2+ -dependent exocytosis similar to neurons 8–10 . However, the existence of this mechanism has been questioned 11–13 owing to inconsistent data 14–17 and a lack of direct supporting evidence. Here we revisited the astrocyte glutamate exocytosis hypothesis by considering the emerging molecular heterogeneity of astrocytes 18–21 and using molecular, bioinformatic and imaging approaches, together with cell-specific genetic tools that interfere with glutamate exocytosis in vivo. By analysing existing single-cell RNA-sequencing databases and our patch-seq data, we identified nine molecularly distinct clusters of hippocampal astrocytes, among which we found a notable subpopulation that selectively expressed synaptic-like glutamate-release machinery and localized to discrete hippocampal sites. Using GluSnFR-based glutamate imaging 22 in situ and in vivo, we identified a corresponding astrocyte subgroup that responds reliably to astrocyte-selective stimulations with subsecond glutamate release events at spatially precise hotspots, which were suppressed by astrocyte-targeted deletion of vesicular glutamate transporter 1 (VGLUT1). Furthermore, deletion of this transporter or its isoform VGLUT2 revealed specific contributions of glutamatergic astrocytes in cortico-hippocampal and nigrostriatal circuits during normal behaviour and pathological processes. By uncovering this atypical subpopulation of specialized astrocytes in the adult brain, we provide insights into the complex roles of astrocytes in central nervous system (CNS) physiology and diseases, and identify a potential therapeutic target.

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