4.8 Article

Deletion of the mu opioid receptor gene in mice reshapes the reward-aversion connectome

Publisher

NATL ACAD SCIENCES
DOI: 10.1073/pnas.1601640113

Keywords

mouse brain connectivity; resting-state functional MRI; diffusion tensor imaging; mu opioid receptor; reward/aversion network

Funding

  1. French Academy of Sciences
  2. NIH (National Institute on Alcohol Abuse and Alcoholism) [16658]
  3. Centre National de la Recherche Scientifique, Institut National de la Sante et de la Recherche Meicale
  4. Strasbourg University
  5. Brain Links Brain Tools cluster of excellence from Freiburg (MouseNet)
  6. European Research Area Network (ERANET-Neuron) [AF12-NEUR0008-01-WM2NA]

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Connectome genetics seeks to uncover how genetic factors shape brain functional connectivity; however, the causal impact of a single gene's activity on whole-brain networks remains unknown. We tested whether the sole targeted deletion of the mu opioid receptor gene (Oprm1) alters the brain connectome in living mice. Hypothesis-free analysis of combined resting-state fMRI diffusion tractography showed pronounced modifications of functional connectivity with only minor changes in structural pathways. Fine-grained resting-state fMRI mapping, graph theory, and intergroup comparison revealed Oprm1-specific hubs and captured a unique Oprm1 gene-to-network signature. Strongest perturbations occurred in connectional patterns of pain/aversion-related nodes, including the mu receptor-enriched habenula node. Our data demonstrate that the main receptor for morphine predominantly shapes the so-called reward/aversion circuitry, with major influence on negative affect centers.

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