Modulation of orbitofrontal-striatal reward activity by dopaminergic functional polymorphisms contributes to a predisposition to alcohol misuse in early adolescence

Author:

Baker Travis E.ORCID,Castellanos-Ryan Natalie,Schumann Gunter,Cattrell Anna,Flor Herta,Nees Frauke,Banaschewski Tobias,Bokde Arun,Whelan Rob,Buechel Christian,Bromberg Uli,Papadopoulos Orfanos Dimitri,Gallinat Juergen,Garavan Hugh,Heinz Andreas,Walter Henrik,Brühl Rüdiger,Gowland Penny,Paus Tomáš,Poustka Luise,Martinot Jean-Luc,Lemaitre Herve,Artiges Eric,Paillère Martinot Marie-Laure,Smolka Michael N.,Conrod Patricia,

Abstract

AbstractBackgroundAbnormalities in reward circuit function are considered a core feature of addiction. Yet, it is still largely unknown whether these abnormalities stem from chronic drug use, a genetic predisposition, or both.MethodsIn the present study, we investigated this issue using a large sample of adolescent children by applying structural equation modeling to examine the effects of several dopaminergic polymorphisms of the D1 and D2 receptor type on the reward function of the ventral striatum (VS) and orbital frontal cortex (OFC), and whether this relationship predicted the propensity to engage in early alcohol misuse behaviors at 14 years of age and again at 16 years of age.ResultsThe results demonstrated a regional specificity with which the functional polymorphism rs686 of the D1 dopamine receptor (DRD1) gene and Taq1A of the ANKK1 gene influenced medial and lateral OFC activation during reward anticipation, respectively. Importantly, our path model revealed a significant indirect relationship between the rs686 of the DRD1 gene and early onset of alcohol misuse through a medial OFC × VS interaction.ConclusionsThese findings highlight the role of D1 and D2 in adjusting reward-related activations within the mesocorticolimbic circuitry, as well as in the susceptibility to early onset of alcohol misuse.

Publisher

Cambridge University Press (CUP)

Subject

Psychiatry and Mental health,Applied Psychology

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