Synchrony between midbrain gene transcription and dopamine terminal regulation is modulated by chronic alcohol drinking

Zahra Z. Farahbakhsh; Katherine M. Holleran; Jonathon P. Sens; Steve C. Fordahl; Madelyn I. Mauterer; Alberto J. López; Verginia C. Cuzon Carlson; Drew D. Kiraly; Kathleen A. Grant; Sara R. Jones; Cody A. Siciliano

doi:10.1038/s41467-025-56715-y

Synchrony between midbrain gene transcription and dopamine terminal regulation is modulated by chronic alcohol drinking

Zahra Z. Farahbakhsh
, Katherine M. Holleran
, Jonathon P. Sens
, Steve C. Fordahl
, Madelyn I. Mauterer
, Alberto J. López
, Verginia C. Cuzon Carlson
, Drew D. Kiraly
, Kathleen A. Grant
, Sara R. Jones
, Cody A. Siciliano

Research output: Contribution to journal › Article › peer-review

2 Scopus citations

Abstract

Alcohol use disorder is marked by disrupted behavioral and emotional states which persist into abstinence. The enduring synaptic alterations that remain despite the absence of alcohol are of interest for interventions to prevent relapse. Here, 28 male rhesus macaques underwent over 20 months of alcohol drinking interspersed with three 30-day forced abstinence periods. After the last abstinence period, we paired direct sub-second dopamine monitoring via ex vivo voltammetry in nucleus accumbens core with RNA-sequencing of the ventral tegmental area. We found persistent augmentation of dopamine transporter function, kappa opioid receptor sensitivity, and putative dynorphin release – all inhibitory regulators which act to decrease extracellular dopamine. Surprisingly, though transcript expression was not altered, the relationship between gene expression and functional readouts of these encoded proteins was highly dynamic and altered by drinking history. These results outline the long-lasting synaptic impact of alcohol use and suggest that assessment of transcript-function relationships is critical for the rational design of precision therapeutics.

Original language	English
Article number	1944
Journal	Nature Communications
Volume	16
Issue number	1
DOIs	https://doi.org/10.1038/s41467-025-56715-y
State	Published - Dec 2025
Externally published	Yes

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Farahbakhsh, Z. Z., Holleran, K. M., Sens, J. P., Fordahl, S. C., Mauterer, M. I., López, A. J., Cuzon Carlson, V. C., Kiraly, D. D., Grant, K. A., Jones, S. R., & Siciliano, C. A. (2025). Synchrony between midbrain gene transcription and dopamine terminal regulation is modulated by chronic alcohol drinking. Nature Communications, 16(1), Article 1944. https://doi.org/10.1038/s41467-025-56715-y

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title = "Synchrony between midbrain gene transcription and dopamine terminal regulation is modulated by chronic alcohol drinking",

abstract = "Alcohol use disorder is marked by disrupted behavioral and emotional states which persist into abstinence. The enduring synaptic alterations that remain despite the absence of alcohol are of interest for interventions to prevent relapse. Here, 28 male rhesus macaques underwent over 20 months of alcohol drinking interspersed with three 30-day forced abstinence periods. After the last abstinence period, we paired direct sub-second dopamine monitoring via ex vivo voltammetry in nucleus accumbens core with RNA-sequencing of the ventral tegmental area. We found persistent augmentation of dopamine transporter function, kappa opioid receptor sensitivity, and putative dynorphin release – all inhibitory regulators which act to decrease extracellular dopamine. Surprisingly, though transcript expression was not altered, the relationship between gene expression and functional readouts of these encoded proteins was highly dynamic and altered by drinking history. These results outline the long-lasting synaptic impact of alcohol use and suggest that assessment of transcript-function relationships is critical for the rational design of precision therapeutics.",

author = "Farahbakhsh, \{Zahra Z.\} and Holleran, \{Katherine M.\} and Sens, \{Jonathon P.\} and Fordahl, \{Steve C.\} and Mauterer, \{Madelyn I.\} and L{\'o}pez, \{Alberto J.\} and \{Cuzon Carlson\}, \{Verginia C.\} and Kiraly, \{Drew D.\} and Grant, \{Kathleen A.\} and Jones, \{Sara R.\} and Siciliano, \{Cody A.\}",

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AU - Fordahl, Steve C.

AU - Mauterer, Madelyn I.

AU - López, Alberto J.

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AU - Kiraly, Drew D.

AU - Grant, Kathleen A.

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AB - Alcohol use disorder is marked by disrupted behavioral and emotional states which persist into abstinence. The enduring synaptic alterations that remain despite the absence of alcohol are of interest for interventions to prevent relapse. Here, 28 male rhesus macaques underwent over 20 months of alcohol drinking interspersed with three 30-day forced abstinence periods. After the last abstinence period, we paired direct sub-second dopamine monitoring via ex vivo voltammetry in nucleus accumbens core with RNA-sequencing of the ventral tegmental area. We found persistent augmentation of dopamine transporter function, kappa opioid receptor sensitivity, and putative dynorphin release – all inhibitory regulators which act to decrease extracellular dopamine. Surprisingly, though transcript expression was not altered, the relationship between gene expression and functional readouts of these encoded proteins was highly dynamic and altered by drinking history. These results outline the long-lasting synaptic impact of alcohol use and suggest that assessment of transcript-function relationships is critical for the rational design of precision therapeutics.

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Synchrony between midbrain gene transcription and dopamine terminal regulation is modulated by chronic alcohol drinking

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