# The interaction of DA\glutamate signaling in vulnerability to aberrant alcohol seeking

> **NIH NIH P50** · YALE UNIVERSITY · 2020 · $275,193

## Abstract

Project 1: The Interaction of DA/Glutamate Signaling in Vulnerability to Aberrant Alcohol Seeking
Jane Taylor, Ph.D.
Abstract
Although many people can casually consume alcohol, some people develop alcohol use disorder (AUD),
especially those that are family history positive (FHP) for AUD. In AUD, drinking becomes habitual and alcohol
cues become powerful triggers that invigorate alcohol seeking and ultimately trigger relapse to alcohol
consumption. Unfortunately, there are few effective therapies that reduce the strength of these cues. Our goal
is to use cutting edge behavioral, transgenic and viral techniques to provide a more complete understanding of
the neurobiological mechanisms of habitual alcohol seeking and relapse. We will test the overarching
hypothesis that habitual alcohol seeking and relapse in FHP and AUD is due to enhanced D1-R-mediated
NMDA-R function and decreased D2-R-mediated NMDA-R function in the dorsal striatum. In CTNA3 we found
that vulnerability to habitual ethanol (EtOH) seeking and relapse in mice was associated with two distinct
endophenotypes of enhanced cue reactivity. First, mice that exhibited high Pavlovian Approach (PA) exhibited
greater habitual alcohol seeking relative to mice that exhibited low PA. Second, mice that exhibited high
Pavlovian to Instrumental Transfer (PIT) exhibited greater cue-induced reinstatement of EtOH seeking relative
to mice that exhibited low PIT. Here, we will study the molecular basis of these predictors of compulsive EtOH
seeking. Specifically, we propose to investigate the role of DA signaling cascades that underlie the transition
from goal-directed to habitual alcohol seeking (Aim 1), and cue-induced relapse (Aim 2). We will use cell-
specific viral knockdown of the key DA-signaling molecules that regulate NMDA-R function, the tyrosine kinase
Fyn and the tyrosine phosphatase STEP, in D1-Cre and D2/A2A-Cre mice to selectively determine the roles of
Fyn and STEP in D1 or D2 dorso-medial and dorso-lateral striatal neurons: The AAV-flox-Fyn-shRNA and
AAV-flox-STEP-shRNA constructs were designed specifically for this project. We will then test a novel
systemic Fyn inhibitor to prevent the transition to habitual EtOH-seeking. In CTNA3, we also found that cortical
neural cell adhesion molecule (NCAM) expression predicted cue-reactivity and was required for cessation of
EtOH-seeking behaviors. The Clinical Core identified NCAM-1 as the gene most closely associated with Fyn
kinase in the AUD “risk” gene network. We will investigate dorso-striatal NCAM signaling-dependent NMDA-R
expression in the regulation of habitual alcohol seeking and relapse through enhanced polysialation: The AAV-
PST virus is a novel means to enhance PSA-NCAM expression. Finally, we are uniquely positioned to study
sex differences in EtOH seeking and DA/NMDA signaling. In CTNA3 we found the transition to habitual EtOH
seeking is accelerated in male mice relative to female mice, and this depends on chromosomal complemen...

## Key facts

- **NIH application ID:** 9941000
- **Project number:** 5P50AA012870-20
- **Recipient organization:** YALE UNIVERSITY
- **Principal Investigator:** Jane R Taylor
- **Activity code:** P50 (R01, R21, SBIR, etc.)
- **Funding institute:** NIH
- **Fiscal year:** 2020
- **Award amount:** $275,193
- **Award type:** 5
- **Project period:** — → —

## Primary source

NIH RePORTER: https://reporter.nih.gov/project-details/9941000

## Citation

> US National Institutes of Health, RePORTER application 9941000, The interaction of DA\glutamate signaling in vulnerability to aberrant alcohol seeking (5P50AA012870-20). Retrieved via AI Analytics 2026-05-23 from https://api.ai-analytics.org/grant/nih/9941000. Licensed CC0.

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