Abstract
Cocaine exposure induces plasticity of glutamatergic synapses of medium spiny neurons (MSNs) in the nucleus accumbens (NAc), which has been proposed to contribute to its addictive behavior. The mechanisms underlying cocaine-induced plasticity are not fully understood. The orphan glutamate delta-1 (GluD1) receptor is a member of the ionotropic glutamate receptor family but does not function as a typical ligand-gated ion channel. Instead it serves a synaptogenic function by interacting with presynaptic Neurexin protein. Recent neuroanatomical studies have demonstrated enriched expression of GluD1 in the NAc but its role in reward behavior, MSN function, and drug-induced plasticity remains unknown. Using a combination of constitutive and conditional GluD1 KO models, we evaluated the effect of GluD1 ablation on cocaine-conditioned place preference (CPP) and cocaine-induced structural and functional plasticity. GluD1 KO mice showed higher cocaine CPP. Selective ablation of GluD1 from striatal neurons but not cortico-limbic excitatory neurons reproduced higher CPP. Higher cocaine preference in GluD1 KO correlated with an increase in spine density, greater maturation of dendritic spines, and basally upregulated spine-regulating active cofilin. GluD1 loss did not affect basal excitatory neurotransmission or plasticity but masked the generation of cocaine-induced silent synapses. Finally, loss of GluD1 increased the GluN2B subunit contribution to NMDA receptor currents in MSNs and a partial agonist of GluN2B-containing NMDA receptors normalized the higher active cofilin and cocaine preference in GluD1 KO mice. Together, these findings demonstrate a critical role of GluD1 in controlling susceptibility to cocaine preference and cocaine-induced plasticity by modulating NMDA receptor subunit contribution.
Highlights
Cocaine-induced neuroplasticity in the nucleus accumbens (NAc) has been proposed to contribute to its addictive behavior
We found that glutamate delta-1 (GluD1) KO mice spent significantly more time on the cocaine (5 mg/kg) injected side compared to wildtype (WT 67.13 ± 21.86 s vs. GluD1 KO 165.2 ± 37.48 s, p = 0.033, unpaired t-test)
We observed a significant increase in total spine density in NAc core medium spiny neurons (MSNs) in GluD1 KO but not in wildtype mice exposed to cocaine compared to saline controls
Summary
Cocaine-induced neuroplasticity in the nucleus accumbens (NAc) has been proposed to contribute to its addictive behavior. Plasticity in dendritic spines of medium spiny neurons (MSNs) and glutamatergic neurotransmission is observed after cocaine exposure[1,2,3,4,5,6,7,8]. An increase in the active form of cofilin is observed upon cocaine exposure and constitutively active cofilin and dominant negative Rac[1] increase cocaine preference[9]. Cocaine exposure has been found to induce generation of silent synapses in MSNs5,10 and impairing maturation of silent synapses reverses incubation of cocaine craving[11,12]. Generation of silent synapses, which contain NMDA receptors but lack AMPA receptors, correlates with an increase in the expression of GluN2B subunit[10]. The role of several intracellular PSD components has been evaluated to account for these functional changes in synapses[13,14,15]; the role of synaptogenic factors, such as adhesion molecules, is still lacking
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