4.8 Article

Reducing Astrocyte Calcium Signaling In Vivo Alters Striatal Microcircuits and Causes Repetitive Behavior

Journal

NEURON
Volume 99, Issue 6, Pages 1170-+

Publisher

CELL PRESS
DOI: 10.1016/j.neuron.2018.08.015

Keywords

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Categories

Funding

  1. NIH [NS060677, MH104069]
  2. Shirley and Stefan Hatos Foundation
  3. NINDS Informatics Center for Neurogenetics and Neurogenomics [P30 NS062691]
  4. Genetics, Genomics, and Informatics Core of the Semel Institute of Neuroscience at UCLA
  5. Eunice Kennedy Shriver National Institute of Child Health and Human Development [U54HD087101-01]
  6. American Heart Association [16POST27260256]
  7. JSPS Overseas Research Fellowship [H28-729]
  8. [U01NS094286]
  9. [K99DA004016]
  10. [DA005010]

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Astrocytes tile the central nervous system, but their functions in neural microcircuits in vivo and their roles in mammalian behavior remain incompletely defined. We used two-photon laser scanning microscopy, electrophysiology, MINIscopes, RNA-seq, and a genetic approach to explore the effects of reduced striatal astrocyte Ca2+ signaling in vivo. In wild-type mice, reducing striatal astrocyte Ca2+-dependent signaling increased repetitive self-grooming behaviors by altering medium spiny neuron (MSN) activity. The mechanism involved astrocyte-mediated neuromodulation facilitated by ambient GABA and was corrected by blocking astrocyte GABA transporter 3 (GAT-3). Furthermore, in a mouse model of Huntington's disease, dysregulation of GABA and astrocyte Ca2+ signaling accompanied excessive self-grooming, which was relieved by blocking GAT-3. Assessments with RNA-seq revealed astrocyte genes and pathways regulated by Ca2+ signaling in a cell-autonomous and non-cell-autonomous manner, including Rab11a, a regulator of GAT-3 functional expression. Thus, striatal astrocytes contribute to neuromodulation controlling mouse obsessive-compulsive-like behavior.

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