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Publication : A disinhibitory microcircuit of the orbitofrontal cortex mediates cocaine preference in mice.

First Author  Huang Z Year  2024
Journal  Mol Psychiatry Volume  29
Issue  10 Pages  3160-3169
PubMed ID  38698268 Mgi Jnum  J:359482
Mgi Id  MGI:7788299 Doi  10.1038/s41380-024-02579-5
Citation  Huang Z, et al. (2024) A disinhibitory microcircuit of the orbitofrontal cortex mediates cocaine preference in mice. Mol Psychiatry 29(10):3160-3169
abstractText  Both clinical and animal studies showed that the impaired functions of the orbitofrontal cortex (OFC) underlie the compulsive drug-seeking behavior of drug addiction. However, the functional changes of the microcircuit in the OFC and the underlying molecular mechanisms in drug addiction remain elusive, and little is known for whether microcircuits in the OFC contributed to drug addiction-related behaviors. Utilizing the cocaine-induced conditioned-place preference model, we found that the malfunction of the microcircuit led to disinhibition in the OFC after cocaine withdrawal. We further showed that enhanced Somatostatin-Parvalbumin (SST-PV) inhibitory synapse strength changed microcircuit function, and SST and PV inhibitory neurons showed opposite contributions to the drug addiction-related behavior of mice. Brevican of the perineuronal nets of PV neurons regulated SST-PV synapse strength, and the knockdown of Brevican alleviated cocaine preference. These results reveal a novel molecular mechanism of the regulation of microcircuit function and a novel circuit mechanism of the OFC in gating cocaine preference.
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