4.2 Article

Differential Response of Glial Fibrillary Acidic Protein-Positive Astrocytes in the Rat Prefrontal Cortex Following Ethanol Self-Administration

Journal

ALCOHOLISM-CLINICAL AND EXPERIMENTAL RESEARCH
Volume 39, Issue 4, Pages 650-658

Publisher

WILEY
DOI: 10.1111/acer.12683

Keywords

Astrocyte; Glial Fibrillary Acidic Protein; Self-Administration; Stereology; Prefrontal Cortex

Funding

  1. AMBRF/Foundation for Alcohol Research
  2. NIH/NIAAA [P50 AA022537]
  3. NIH/NCATS [UL1 TR000058]
  4. [NIAAA/P30-AA019372]

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BackgroundPrefrontal cortex (PFC) dysfunction is believed to contribute to the transition from controlled substance use to abuse. Because astrocytes have been suggested to play a key role in the development and maintenance of drug-seeking behaviors, we sought to determine whether PFC astrocytes are affected by ethanol (EtOH) self-administration. MethodsEtOH consumption was modeled in rats by 3 self-administration paradigms where EtOH was made concurrently available with water in the home cage either continuously (CEA) or intermittently (IEA). In the third paradigm, EtOH was only available in the operant chamber (OEA). To avoid the potential confound of acute EtOH effects, all rats were sacrificed after either 24-hour or 3-week abstinence. In all groups, the effect of EtOH consumption on PFC astrocytes was measured using unbiased stereological counting of cells expressing the astrocyte marker glial fibrillary acidic protein (GFAP). GFAP immunoreactivity commonly changes in response to pharmacological insult or injury. ResultsGFAP-positive astrocyte number increased in the prelimbic and anterior cingulate cortex regions of the PFC after IEA. No change was found in the infralimbic or orbitofrontal cortex after IEA. After 3-week abstinence, there was a reduction of astrocytes in the prelimbic and orbitofrontal cortex of the CEA cohort as well as a reduction in the orbitofrontal cortex of the OEA cohort. ConclusionsThese findings demonstrate that discrete PFC subregions contain GFAP-positive astrocyte populations that respond differentially to distinct EtOH consumption paradigms. A better understanding of how specific astrocyte populations uniquely adapt to EtOH consumption could provide insight for targeted therapeutic interventions.

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