Intravenous Ketamine in the Treatment of Obsessive-Compulsive Disorder
Status:
Terminated
Trial end date:
2015-06-01
Target enrollment:
Participant gender:
Summary
Obsessive-Compulsive Disorder (OCD) is a chronic and disabling anxiety disorder and a leading
cause of worldwide disability that presents a significant public health problem. Treatment
options are limited and many OCD patients fail to respond completely or quickly to standard
treatments, including pharmacotherapy and psychotherapy. At this time, patients who fail to
respond to treatment with serotonergic drugs, augmenting antipsychotic agents, and behavioral
therapy, have few additional treatment options aside from deep brain stimulation. Therefore,
despite advances in current pharmacological and behavioral treatments, and the utility of
serotonergic drugs, it is likely that other neurotransmitter systems are involved and that
targeting these systems may increase treatment efficacy. Despite little evidence for
serotonergic dysfunction in OCD, there is significant evidence that glutamatergic
dysregulation may contribute to the development and progression of the disorder. Also,
preliminary studies suggest that glutamatergic modulators (i.e. riluzole and d-cycloserine),
particularly agents acting at the NMDA receptor (i.e. memantine), may be useful in OCD. The
NMDA antagonist, ketamine, has demonstrated rapid effects when delivered as a single
intravenous (IV) dose in depressed patients. Therefore, the objective of the current study is
to investigate the safety and efficacy of a single dose of IV ketamine in treatment-resistant
OCD.