Recent data suggest that obsessive-compulsive disorder(OCD)is driven by an imbalance among the habit learning system and the goal-directed system.The frontostriatal loop termed cortico-striatal-thalamo-cortical(CSTC)c...Recent data suggest that obsessive-compulsive disorder(OCD)is driven by an imbalance among the habit learning system and the goal-directed system.The frontostriatal loop termed cortico-striatal-thalamo-cortical(CSTC)circuitry loop is involved in habits and their dysfunction plays an important role in OCD.Glutamatergic neurotransmission is the principal neurotransmitter implicated in the CSTC model of OCD.Hyperactivity in the CSTC loop implies a high level of glutamate in the cortical-striatal pathways as well as a dysregulation of GABA ergic transmission,and could represent the pathophysiology of OCD.Moreover,the dysregulation of glutamate levels can lead to neurotoxicity,acting as a neuronal excitotoxin.The hypothesis of a role of neurotoxicity in the pathophysiology of OCD clinically correlates to the importance of an early intervention for patients.Indeed,some studies have shown that a reduction of duration of untreated illness is related to an earlier onset of remission.Although robust data supporting a progression of such brain changes are not available so far,an early intervention could help interrupt damage from neurotoxicity.Moreover,agents targeting glutamate neurotransmission may represent promising therapeutical option in OCD patients.展开更多
文摘Recent data suggest that obsessive-compulsive disorder(OCD)is driven by an imbalance among the habit learning system and the goal-directed system.The frontostriatal loop termed cortico-striatal-thalamo-cortical(CSTC)circuitry loop is involved in habits and their dysfunction plays an important role in OCD.Glutamatergic neurotransmission is the principal neurotransmitter implicated in the CSTC model of OCD.Hyperactivity in the CSTC loop implies a high level of glutamate in the cortical-striatal pathways as well as a dysregulation of GABA ergic transmission,and could represent the pathophysiology of OCD.Moreover,the dysregulation of glutamate levels can lead to neurotoxicity,acting as a neuronal excitotoxin.The hypothesis of a role of neurotoxicity in the pathophysiology of OCD clinically correlates to the importance of an early intervention for patients.Indeed,some studies have shown that a reduction of duration of untreated illness is related to an earlier onset of remission.Although robust data supporting a progression of such brain changes are not available so far,an early intervention could help interrupt damage from neurotoxicity.Moreover,agents targeting glutamate neurotransmission may represent promising therapeutical option in OCD patients.
