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Sustaining Remission of Psychotic Depression (STOP-PD)

This study is currently recruiting participants.
Verified March 2013 by Weill Medical College of Cornell University
Sponsor:
Collaborators:
University of Toronto
University of Massachusetts, Worcester
University of Pittsburgh
Information provided by (Responsible Party):
Weill Medical College of Cornell University
ClinicalTrials.gov Identifier:
NCT01427608
First received: August 30, 2011
Last updated: March 11, 2013
Last verified: March 2013
History of Changes

August 30, 2011
March 11, 2013
October 2011
January 2016   (final data collection date for primary outcome measure)
Risk of relapse during the randomized phase. [ Time Frame: From entry into randomized phase until 36 weeks or earlier relapse ] [ Designated as safety issue: No ]

Relapse criteria include at least one of the following:

1)Structured Clinical Interview for Diagnostic Statistical Manual #4 Trade Revision (DSM-IV-TR) Axis 1 Disorders (SCID) symptoms of major depression maintained over two weeks 2)17-item Hamilton Depression (HAM-D)score of >17 maintained for more than one week + a mean increase of 5 points from entry into randomized phase 3)Re-emergence of psychosis for more than one week, with a score of >2 on delusion or hallucination severity items 4)Significant clinical worsening defined as either emergence of high-risk of suicide, and/or development of mania for greater than one week, and/or psychiatric hospitalization.
Risk of relapse during the randomized phase. [ Time Frame: From entry into randomized phase until 36 weeks or earlier relapse ] [ Designated as safety issue: No ]

Relapse criteria include at least one of the following:

1)SCID symptoms of major depressive episode maintained over two weeks 2)17-item HAM-D score of >17 maintained for more than one week + a mean increase of 5 points from entry into randomized phase 3)Re-emergence of SCID defined psychosis for more than one week, with a score of >2 on SADS delusion or hallucination severity items 4)Significant clinical worsening defined as either emergence of high-risk of suicide, and/or development of mania for greater than one week, and/or psychiatric hospitalization.
Complete list of historical versions of study NCT01427608 on ClinicalTrials.gov Archive Site
Changes in metabolic measures [ Time Frame: From entry into randomized phase until up to 36 weeks later ] [ Designated as safety issue: Yes ]
Weight and clinical laboratory analyses of cholesterol and triglycerides
Same as current
Age differences in treatment response Under60/60 or older [ Time Frame: 36 weeks ] [ Designated as safety issue: Yes ]
Metabolic changes and symptom response will be compared for 'old' versus 'young'
Not Provided
 
Sustaining Remission of Psychotic Depression
Sustaining Remission of Psychotic Depression

The acute phase of this study will monitor the response to a combination of an atypical antipsychotic medication olanzapine with an antidepressant medication sertraline in the acute treatment of the disorder. It is predicted that this combination will improve symptoms of psychotic depression and be associated metabolic side effects. Factors that moderate tolerability will be monitored. Improvement in symptoms could take between 4 and 12 weeks, followed by a period of 8 weeks during which participants will continue to take the same medications to stabilize the remission from symptoms of psychotic depression.

The maintenance phase will be a randomized, double-blind, placebo-controlled study of olanzapine for a period of up to 36 weeks to test whether continuing this combination decreases the risk of relapse and whether discontinuing the combination leads to improvement in metabolic measures. Subjects who complete the acute phase will be asked to consent separately to the randomized maintenance phase.

The original STOP-PD study established that the combination of olanzapine and sertraline was significantly better than olanzapine alone in achieving remission of psychotic depression. This STOP-PD-II Sustaining Remission study aims to assess the long-term tolerability of taking this combination of medications and their efficacy at preventing a relapse of the symptoms. The acute phase of the study will monitor the efficacy and tolerability of the olanzapine and sertraline combination, including investigation of weight and metabolic variables, age effects on treatment response and tolerability, and the association of genetic polymorphisms to response or relapse. When subjects are stabilized on these medications for a period of 8 weeks they will be invited to participate in the randomized phase of the research: the olanzapine will be placebo-controlled, meaning half of the subjects will continue to take the olanzapine/sertraline combination and half will take a sertraline/placebo combination, for a period of 36 weeks. Symptoms and side effects will be monitored regularly throughout this phase. Randomization will be stratified on a 1:1 basis by age 60 and above.
Interventional
Phase 4
Allocation: Randomized
Endpoint Classification: Safety/Efficacy Study
Intervention Model: Parallel Assignment
Masking: Double Blind (Subject, Caregiver, Investigator, Outcomes Assessor)
Primary Purpose: Treatment
Psychotic Depression
  • Drug: Olanzapine
    Olanzapine 15mg/day. Adjustment of dose to 5mg/day to a maximum of 20mg/day will be permitted if necessitated by significant side-effects or clinical worsening
    Other Name: Zyprexa
  • Drug: Placebo
    Taper from current dose of olanzapine to placebo over 4 weeks. Continue placebo for remainder of 36 week study.
  • Active Comparator: Olanzapine
    Olanzapine 15mg/day plus sertraline 150mg/day. Fluctuations in dosing are allowed up to a maximum of olanzapine 20mg/day, sertraline 200mg/day.
    Intervention: Drug: Olanzapine
  • Placebo Comparator: Placebo
    Placebo will be used to taper the olanzapine over a period of four weeks and then substitute for the olanzapine for the remainder of the 36 week study.
    Intervention: Drug: Placebo
Flint AJ, Meyers BS, Rothschild AJ, Whyte EM, Mulsant BH, Rudorfer MV, Marino P; STOP-PD II Study Group. Sustaining remission of psychotic depression: rationale, design and methodology of STOP-PD II. BMC Psychiatry. 2013 Jan 25;13:38. doi: 10.1186/1471-244X-13-38.

*   Includes publications given by the data provider as well as publications identified by ClinicalTrials.gov Identifier (NCT Number) in Medline.
 
Recruiting
392
June 2016
January 2016   (final data collection date for primary outcome measure)

Inclusion Criteria:

  1. Aged 18-85 years, inclusive
  2. Diagnosis: Diagnostic Statistical Manual-IV Trade Revision (DSM IV-TR) non-bipolar major depression with psychotic features established by both clinical interview with research psychiatrist and administration of SCID-IV.
  3. Score >2 on Schedule for Affective Disorders (SADS) delusion severity item
  4. Score >1 on any of the three conviction items of the Delusion Assessment Scale (DAS) (does not alter belief in response to reality testing)
  5. 17-item HAM-D score of >20

Exclusion Criteria:

  1. Current or lifetime DSM-IV-TR history of schizophrenia or other psychotic disorders or meeting current criteria for brief psychotic disorder, body dysmorphic disorder or obsessive-compulsive disorder
  2. Current or lifetime DSM-IV-TR bipolar affective disorder
  3. History of DSM-IV-TR defined alcohol or substance abuse or dependence within the past three months
  4. Dementia or clinically significant cognitive impairment prior to index episode of depression, and/or a mean score >3 on 26-item caregiver assessment
  5. Type 1 diabetes mellitus (defined as insulin-dependent diabetes mellitus with onset before age 35, and/or diabetes mellitus complicated by prior documented episode of ketoacidosis
  6. Acute or unstable medical illness within the past 3 months; current abnormal serum free T4; current abnormally low vitamin B4 or folic acid level; medical conditions and/or medications for which psychotic or depressive symptoms can be a direct manifestation; neurological disease associated with extrapyramidal signs and symptoms; epilepsy, if the person has had one or more grand mal seizures within the past 12 months.
  7. The need for treatment with any psychotropic medication other than sertraline, olanzapine or lorazepam; or with an anticonvulsant medication with mood-stabilizing properties.
  8. Current pregnancy or plan to become pregnant during the course of the study; breast feeding in women with infants.
  9. A documented history of being unable to tolerate olanzapine or sertraline including significant bradycardia (heart rate of <50 bpm), and serum sodium level of 129mmol/L or below.
  10. History of non-response of the index episode of psychotic depression to at least a 6-week trial of at least 150mg/day sertraline combined with 15mg/day olanzapine
  11. Patients showing ongoing improvement in current episode of psychotic depression with treatment other than sertraline or olanzapine
  12. Patients who are in immediate need of electroconvulsive therapy (ECT) (imminent risk of suicide, refusing to eat, catatonic)
Both
18 Years to 85 Years
No
Not Provided
United States,   Canada
 
NCT01427608
STOP-PD-II
Yes
Weill Medical College of Cornell University
Weill Medical College of Cornell University
  • University of Toronto
  • University of Massachusetts, Worcester
  • University of Pittsburgh
Principal Investigator: Barnett S Meyers, MD Weill Medical College of Cornell University
Principal Investigator: Alastair Flint, MD University of Toronto
Principal Investigator: Anthony Rothschild, MD University of Massachusetts, Worcester
Principal Investigator: Ellen Whyte, MD University of Pittsburgh
Weill Medical College of Cornell University
March 2013

ICMJE     Data element required by the International Committee of Medical Journal Editors and the World Health Organization ICTRP