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Insulin regulates astrocyte gliotransmission and modulates behavior.

Citation
Cai, W., et al. “Insulin Regulates Astrocyte Gliotransmission And Modulates Behavior.”. The Journal Of Clinical Investigation, pp. 2914-2926.
Center Joslin Diabetes Center
Author Weikang Cai, Chang Xue, Masaji Sakaguchi, Masahiro Konishi, Alireza Shirazian, Heather A Ferris, Mengyao E Li, Ruichao Yu, André Kleinridders, Emmanuel N Pothos, Ronald Kahn
Keywords depression, diabetes, Insulin Signaling, Metabolism, neuroscience
Abstract

Complications of diabetes affect tissues throughout the body, including the central nervous system. Epidemiological studies show that diabetic patients have an increased risk of depression, anxiety, age-related cognitive decline, and Alzheimer's disease. Mice lacking insulin receptor (IR) in the brain or on hypothalamic neurons display an array of metabolic abnormalities; however, the role of insulin action on astrocytes and neurobehaviors remains less well studied. Here, we demonstrate that astrocytes are a direct insulin target in the brain and that knockout of IR on astrocytes causes increased anxiety- and depressive-like behaviors in mice. This can be reproduced in part by deletion of IR on astrocytes in the nucleus accumbens. At a molecular level, loss of insulin signaling in astrocytes impaired tyrosine phosphorylation of Munc18c. This led to decreased exocytosis of ATP from astrocytes, resulting in decreased purinergic signaling on dopaminergic neurons. These reductions contributed to decreased dopamine release from brain slices. Central administration of ATP analogs could reverse depressive-like behaviors in mice with astrocyte IR knockout. Thus, astrocytic insulin signaling plays an important role in dopaminergic signaling, providing a potential mechanism by which astrocytic insulin action may contribute to increased rates of depression in people with diabetes, obesity, and other insulin-resistant states.

Year of Publication
2018
Journal
The Journal of clinical investigation
Volume
128
Issue
7
Number of Pages
2914-2926
Date Published
12/2018
ISSN Number
1558-8238
DOI
10.1172/JCI99366
Alternate Journal
J. Clin. Invest.
PMID
29664737
PMCID
PMC6025980
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