Trial | NCT02083926  Report issue

Official Title

Ketamine Infusion for Social Anxiety Disorder

  • Phase

    Early Phase 1

  • Study Type

    Interventional

  • Study Participants

    18
Social Anxiety Disorder (SAD) is common and causes significant impairment.
First-line treatments for Social Anxiety Disorder are only partially effective. Many SAD patients experience little or inadequate symptom relief with available treatments.
Ketamine is a potent NMDA receptor antagonist. Ketamine represents an agent with a potentially novel mechanism of action for the treatment of anxiety disorders.
Ketamine has demonstrated efficacy in the treatment of psychiatric disorders closely related to Social Anxiety Disorder including Major Depression, Bipolar Depression and possibly Obsessive-Compulsive Disorder.

Ketamine represents the possibility to provide rapid symptom relief to patients with SAD and may provide the mechanism for future drug development to treat SAD more rapidly and effectively.
Roughly one-third to one-half of patients with generalized SAD do not experience significant clinical benefit from current evidence-based treatment for SAD such as pharmacotherapy with selective serotonin reuptake inhibitors (SSRI) or venlafaxine and cognitive behavioral therapy (CBT). Failure of anxiety relief in patients with SAD is a source of substantial morbidity, distress, and decreases in quality of life. Novel pharmacological treatments are needed to improve patient outcomes with SAD.

Converging lines of evidence from neuroimaging and pharmacological studies support the importance of glutamate abnormalities in the pathogenesis of SAD. In a Magnetic Resonance Spectroscopy (MRS) study, an elevated glutamate to creatinine ratio was found in the anterior cingulate cortex of SAD patients when compared to healthy controls. Elevated thalamic glutamine levels have been demonstrated in patients with SAD. Pre-clinical rodent studies have also established a strong link between glutamate regulation and anxiety.

Ketamine is a potent antagonist of the N-methyl-D-aspartate (NMDA) receptor, a major type of glutamate receptor in the brain. Ketamine is routinely used for anesthetic induction because of its dissociative properties. However in research studies, ketamine is effective treatment in reducing symptoms in depressive and possibly anxiety disorders. In multiple controlled clinical studies, ketamine has produced a rapid antidepressant effect in unipolar and bipolar depression. Ketamine's anti-depressant effects peak 1-3 days following infusion. Ketamine's antidepressant effect is observed long after ketamine has been metabolized and excreted by the body and after ketamine's sedative and dissociative effects have dissipated.

The results of several clinical studies suggest that ketamine may also have significant anxiolytic effects. Patients with major depressive disorder given a single ketamine infusion have shown strong and significant reductions in comorbid anxiety symptoms. A trial including 11 depressed patients demonstrated a significant reduction in anxiety symptoms (Hamilton Anxiety Rating Scale (HAM-A)) following ketamine infusion. This improvement is supported by one of the earlier placebo-controlled trials of ketamine which demonstrated that the psychic anxiety item was one of 4 (out of 21) items on the Hamilton Depression Rating Scale (HAM-D) demonstrating significant improvement after ketamine infusion.

The investigators goal is to conduct a randomized, placebo-controlled crossover study to explore the efficacy and time course of action of intravenous ketamine in the treatment of SAD.
Study Started
Jan 02
2015
Primary Completion
Sep 27
2016
Study Completion
Sep 27
2016
Results Posted
Mar 18
2021
Last Update
Mar 18
2021

Drug Ketamine

Ketamine (a single 0.5mg/kg intravenously over 40 minutes).

  • Other names: Ketalar

Other Saline

Saline (a single 0.5mg/kg intravenously over 40 minutes).

  • Other names: Placebo

Ketamine infusion Experimental

A ketamine infusion was given on day 0 (28) at a dose of 0.5mg/kg over 40 minutes. Assessments were conducted pre-infusion, 3-h post-infusion, and days 1 (1+28), 2 (2+28), 3 (3+28), 5 (5+28), 7 (7+28), 10 (10+28) and 14 (14+28) post-infusion.

Saline infusion Experimental

A saline infusion was given on day 0 (28) at a dose of 0.5mg/kg over 40 minutes. Assessments were conducted pre-infusion, 3-h post-infusion, and days 1 (1+28), 2 (2+28), 3 (3+28), 5 (5+28), 7 (7+28), 10 (10+28) and 14 (14+28) post-infusion.

Criteria 

Inclusion Criteria:

Adult between the ages of 18 and 65 years
Meet DSM IV criteria for Social Anxiety Disorder by structured clinical interview (SCID) and have a LSAS >60 with or without co-morbid MDD

Exclusion Criteria:

Positive pregnancy test
History of substance abuse disorder within the last 6 months or positive urine toxicology on screening (within the previous 6 months).
History of pervasive developmental disorder or psychotic disorder by DSM-IV-TR criteria
Medical comorbidity that significantly increases the risks associated with ketamine infusion (e.g. untreated hypertension, significant cardiovascular disease)

Summary

Ketamine Infusion on Day 0 or Day 28

Saline Infusion on Day 0 or Day 28

All Events

Event Type Organ System Event Term Ketamine Infusion on Day 0 or Day 28 Saline Infusion on Day 0 or Day 28

Visual Analogue Scale for Anxiety Symptoms (VAS-anxiety)

Instrument that tries to measure anxiety, that is believed to range across a continuum of values and cannot easily be directly measured.We used a straight horizontal line of 100 mm in length. The ends were defined as the extreme limits of the parameter to be measured (anxiety); oriented from the left (no anxiety) to the right (worst anxiety ever felt). The patient marks on the line the point that they feel represents their perception of their current state.The VAS score is determined by measuring in millimeters from the left hand end of the line to the point that the patient marks. We examined Visual Analog Scale (VAS) for anxiety symptoms at screening, 1 hour prior to infusion, 1, 2 and 3 hours after infusion, 1, 2, 3, 5, 7, 10, and 14 days following a single ketamine/saline infusion.

Ketamine Infusion on Day 0 or Day 28

12.1
units on a scale (Mean)
Standard Deviation: 18.6

Saline Infusion on Day 0 or Day 28

19.6
units on a scale (Mean)
Standard Deviation: 18.5

Liebowitz Social Anxiety Score (LSAS)

Clinician-administered scale for the assessment of fear and avoidance found in social phobia (SAD); it has 24 items divided into 2 subscales, 13 for performance anxiety, and 11 for social situations each rated from 0 to 3 (0=none,1=mild,2=moderate,3=definite). The sum scores for Fear and Avoidance results in an overall score (max 144 points). There are 4 clinician subscales: fear of social interaction, fear of performance, avoidance of social interaction and avoidance of performance 0 to 30= SAD is unlikely 30 to 60=SAD is probable 60 to 90=SADis very probable >90= SAD highly probable

Ketamine Infusion on Day 0 or Day 28

66.1
score on a scale (Mean)
Standard Deviation: 30.9

Saline Infusion on Day 0 or Day 28

86.1
score on a scale (Mean)
Standard Deviation: 30

Total

18
Participants

Age, Continuous

29.72
years (Mean)
Standard Deviation: 11.05

Liebowitz Social Anxiety Score (LSAS)

90.67
units on a scale (Mean)
Standard Deviation: 16.94

Visual Analogue Scale for anxiety symptoms (VAS-anxiety)

47.22
units on a scale (Mean)
Standard Deviation: 18.89

Age, Categorical

Race/Ethnicity, Customized

Region of Enrollment

Sex: Female, Male

Overall Study

Ketamine Infusion on Day 0, Saline Infusion on Day 28

Saline Infusion on Day 0, Ketamine Infusion on Day 28

Drop/Withdrawal Reasons

Ketamine Infusion on Day 0, Saline Infusion on Day 28