Duloxetine Treatment of Major Depression and Chronic Low Back Pain For Older Adults

Last updated: January 30, 2017
Sponsor: University of Pittsburgh
Overall Status: Completed

Phase

4

Condition

Chronic Pain

Depression

Depression (Major/severe)

Treatment

N/A

Clinical Study ID

NCT00696293
KL2RR024154
  • Ages > 60
  • All Genders

Study Summary

The following primary hypotheses will be tested:

  1. During Step 1: Major Depressive Disorder (MDD) or Chronic Low Back Pain (CLBP) in < 40% of the initial 60 subjects treated with duloxetine (DUL) + Clinical Management(CM) during the first 8 weeks will respond (response is defined as a Montgomery Asberg Depression Rating Scale (MADRS) score </=9 and at least a 30% improvement in back pain as measured with the 20-point numeric rating scale.

  2. During Step 2: More DUL+Problem Solving Therapy for Depression and Pain (PST-DP) than DUL+CM treated subjects will achieve response during the second 8 weeks, defined as a MADRS score </=9 and at least a 30% improvement in back pain as measured with the 2-point numeric rating scale.

  3. Improvement in depression scores will be correlated with improvement in CLBP scores.

The exploratory hypotheses to be tested are that:

During Step 2: Compared to subjects treated with DUL+CM, subjects treated with DUL+PST-DP will have improved outcomes in: 1) disability, 2) sleep, 2) functioning/quality of life, 3) caregiver burden/depression, and 5) analgesic use.

Eligibility Criteria

Inclusion

Inclusion Criteria:

  • Age >/= 60

  • Current episode of MDD per SCID DSM-IV criteria

  • Must score >/= 16 on the CES-D assessment

  • Serum sodium >/=130 mEq/ml

  • CLBP of at least moderate severity for more days than not for >/= 3 months

  • MADRS score >/= 15

  • Sufficiently medically stable to be able to participate in a depression treatmentprotocol

  • Willingness and ability to speak English Access to translators is limited. It would beunsafe to treat an older adult who does not speak English with an antidepressant andnot be able to effectively communicate with them about their progress and any sideeffects. We provide a 24/7 on-call service for all subjects enrolled in this study.The on-call clinicians and physicians are not bilingual, and if a problem arose, itmay be impossible to effectively interpret and manage the emergent situation. Finally,many of the assessments used in the study are self-reports. At the present time, we donot have the ability to translate these instruments into other languages. If thesubject cannot read and understand English, this would interfere with their ability tocomplete the self-report assessments

  • Willingness to discontinue other antidepressants and anxiolytics, except for lorazepamup to 2 mg/day

  • Mini Mental State Exam > 20

  • Willingness to provide informed consent

  • Corrected visual ability that enables reading of newspaper headlines and hearingcapacity that is adequate to respond to a raised conversational voice.

Exclusion

Exclusion Criteria:

  • Meet DSM-IV criteria for dementia

  • History of bipolar, schizophrenia, schizoaffective, or other psychotic disorder

  • Alcohol or other drug abuse (including abuse of prescription medications) within thepast 6 months

  • History of treatment non-adherence in other protocols run by the Mid-Life or Late-LifeCenters

  • Acute pain superimposed on chronic pain. For example, subjects who report "red flags"which suggest a herniated disk, vertebral fracture, infection, cauda equina syndrome,or other medical emergency will be excluded

  • Wheelchair bound

  • History of documented non-response to duloxetine

  • Concurrent use of thioridazine

  • Active suicidal ideation with plan

  • Uncontrolled narrow angle glaucoma

Study Design

Total Participants: 30
Study Start date:
May 01, 2007
Estimated Completion Date:
April 30, 2010

Study Description

This is a two-part study. Step 1 is an 8-week long open-label trial of duloxetine (DUL) + clinical management (CM), titrated up to 90 mg/day, for older adults with comorbid major depressive disorder (MDD) and chronic low back pain (CLBP). At week 8, if subjects have not responded, the dose of duloxetine is increased to 120 mg/day. Duloxetine will be increased and continued at 120 mg/day (or highest tolerated dose) for both randomized study groups (during step 2) to assure medication parity.

Step two starts at week 9 and includes those subjects whose MDD and/or CLBP has not met criteria for response during Step 1. At week 9 subjects will be randomized to receive treatment with either: 1) DUL 120 mg/day (or the highest tolerated dose)+ Problem Solving for Depression and Pain (PST-DP) or 2) DUL 120 mg/day (or highest tolerated dose) + CM. Step 2 will be delivered over the course of 8-10 sessions.

NOTE ADDED 1/5/16: THIS WAS TREATMENT DEVELOPMENT WORK CONDUCTED AS PART OF A CAREER DEVELOPMENT AWARD. ONLY THE FIRST OPEN-LABEL PART OF THE STUDY WAS COMPLETED, AND THESE RESULTS HAVE BEEN PUBLISHED AND WILL BE REPORTED HERE ON CLINICALTRIALS.GOV

Connect with a study center

  • University of Pittsburgh School of Medicine

    Pittsburgh, Pennsylvania 15213
    United States

    Site Not Available

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