Abstract

This project addresses the role of astrocytes in regulating neuronal synapses, specifically by regulating levels of AMPA glutamate receptors (AMPARs) at postsynaptic sites. Astrocyte-secreted glypican 4 and 6 (Gpc4&6) are sufficient to induce nascent synapses by clustering calcium-permeable GluA1 AMPA receptors on the postsynaptic dendrite. Further, the mechanism Gpc4 employs is by signaling through presynaptic protein tyrosine phosphatase receptor delta, to induce release of the AMPAR clustering factor neuronal pentraxin 1. In this proposal the mouse visual cortex (VC) will be used to study the relative contribution of astrocyte-expressed glypicans to synapse formation, maturation and plasticity. Preliminary studies showed Gpc4&6 are most highly expressed by astrocytes at the time of synapse formation, fitting with their role inducing nascent synapses, while another astrocyte enriched glypican, Gpc5, is upregulated with synapse maturation and remains high in the adult, suggesting it may regulate synapse maturation or plasticity. This proposal addresses 3 questions related to the role of astrocyte-enriched glypicans in the formation and maturation of excitatory synapses in the VC. 1) What is the role of astrocyte-expressed Gpc5 in synapse maturation and plasticity? Mice lacking Gpc5 in astrocytes have decreased presynaptic size of thalamo-cortical synapses, and altered recruitment of postsynaptic AMPARs. Based on this it is hypothesized that Gpc5 regulates presynaptic maturation, which will be investigated using electrophysiology, immunohistochemistry and electron microscopy. Further, as Gpc4&6 regulate GluA1 AMPARs in development, the hypothesis that Gpc5 is required to increase synaptic levels of GluA1 during plasticity in the adult brain will be tested. 2) What is the role of Gpc4 in excitatory synapse formation onto inhibitory interneurons? Whether astrocytes regulate excitatory synapses onto inhibitory interneurons (INs) is an important unanswered question. As synapses onto INs contain high levels of GluA1 AMPARs, which Gpc4 regulates on principal neurons, it is hypothesized that Gpc4 induces synapses onto INs. Preliminary experiments found a deficit in GluA1 on IN dendrites in the Gpc4 KO. This study will investigate the mechanism underlying this deficit using electrophysiology and immunohistochemistry; ask if the same synaptogenic pathway is employed as at principal neuron synapses; and if lack of Gpc4 affects plasticity at IN synapses. 3) What is the relative contribution of astrocyte-expressed Gpc4&6 to synaptic function? Gpc4&6 are redundant in vitro in inducing synaptic activity. Preliminary studies found Gpc4&6 have different spatial and temporal expression in the developing VC, leading to the hypothesis they have stage and synapse-specific roles in synaptogenesis. This will be analyzed using astrocyte-specific Gpc4 and Gpc6 single KO mice, and astrocyte-specific Gpc4/Gpc6 double KO mice, and synapse formation and function across cortical layers and timepoints examined using electrophysiology and immunohistochemistry. These experiments will reveal region, time and synapse-specific roles of multiple astrocyte glypicans in sculpting neuronal circuit development.

Public Health Relevance

This project identifies the molecular mechanisms used by astrocytes to regulate the development and plasticity of neuronal synapses. Identifying these mechanisms will provide new targets for treatments of neurological disorders caused by synaptic dysfunction, including autism, ADHD, Alzheimer?s disease and schizophrenia.

  Funding Agency

Agency
National Institute of Health (NIH)
Institute
National Institute of Neurological Disorders and Stroke (NINDS)
Type
Research Project (R01)
Project #
2R01NS089791-06
Application #
9819665
Study Section
Cellular and Molecular Biology of Glia Study Section (CMBG)
Program Officer
Leenders, Miriam
Project Start
2014-09-01
Project End
2024-05-31
Budget Start
2019-08-15
Budget End
2020-05-31
Support Year
6
Fiscal Year
2019
Total Cost
Indirect Cost

  Institution

Name
Salk Institute for Biological Studies
Department
Type
DUNS #
078731668
City
La Jolla
State
CA
Country
United States
Zip Code
92037

  Publications

Allen, Nicola J; Lyons, David A (2018) Glia as architects of central nervous system formation and function. Science 362:181-185
Boisvert, Matthew M; Erikson, Galina A; Shokhirev, Maxim N et al. (2018) The Aging Astrocyte Transcriptome from Multiple Regions of the Mouse Brain. Cell Rep 22:269-285
Farhy-Tselnicker, Isabella; Allen, Nicola J (2018) Astrocytes, neurons, synapses: a tripartite view on cortical circuit development. Neural Dev 13:7
Dowling, Cari; Allen, Nicola J (2018) Mice Lacking Glypican 4 Display Juvenile Hyperactivity and Adult Social Interaction Deficits. Brain Plast 4:197-209
Zuidema, Jonathan M; Kumeria, Tushar; Kim, Dokyoung et al. (2018) Oriented Nanofibrous Polymer Scaffolds Containing Protein-Loaded Porous Silicon Generated by Spray Nebulization. Adv Mater 30:e1706785
Bosworth, Alexandra P; Allen, Nicola J (2017) The diverse actions of astrocytes during synaptic development. Curr Opin Neurobiol 47:38-43
Allen, Nicola J; Eroglu, Cagla (2017) Cell Biology of Astrocyte-Synapse Interactions. Neuron 96:697-708
Farhy-Tselnicker, Isabella; van Casteren, Adriana C M; Lee, Aletheia et al. (2017) Astrocyte-Secreted Glypican 4 Regulates Release of Neuronal Pentraxin 1 from Axons to Induce Functional Synapse Formation. Neuron 96:428-445.e13
Blanco-Suárez, Elena; Caldwell, Alison L M; Allen, Nicola J (2017) Role of astrocyte-synapse interactions in CNS disorders. J Physiol 595:1903-1916
Allen, Nicola J (2017) Making Human Stars: A New Method to Generate Human Astrocytes. Neuron 95:725-727

Showing the most recent 10 out of 11 publications