This is a randomised, double-blind, placebo-controlled clinical trial in which patients with major depressive disorder will receive augmentation through minocycline (MCO), celecoxib (CXB) or placebo.
This project aims to repurpose two established anti-inflammatory compounds as adjuvant therapy for immune-mediated depression, in line with state-of-the-art research of the last 10 years. Immune-mediated depression represents a subtype which accounts for approximately 30% of depressive disorders. Patients with this immunosubtype are more likely to have a higher severity of depression, a lower quality of life and more somatic symptoms. Furthermore it is accompanied by a high incidence of treatment resistance. While their mechanisms of action completely differ from those of existing antidepressant treatment options, immunomodulatory drugs celecoxib and minocycline have proven their merit as add-on treatment in depressive episodes. They have been on the Belgian market for years and come with a known pharmacological and safety profile. Patient stratification at baseline based on inflammatory status will reveal which inflammatory subpopulation benefits most from each of the two investigated anti-inflammatory compounds. Additionally, our distinctive study design allows head-to-head comparison of both add-on therapies and will as such provide the last stepping stones towards clinical implementation of individualised treatment strategies in depression.
Study Type
INTERVENTIONAL
Allocation
RANDOMIZED
Purpose
TREATMENT
Masking
QUADRUPLE
Enrollment
240
Oral capsule, 200 mg, twice daily, for 12 weeks
Oral capsule, 100 mg, twice daily, for 12 weeks
Oral capsule, no active substance, twice daily, for 12 weeks
UPC Duffel
Duffel, Antwerpen, Belgium
RECRUITINGUZ Brussel
Brussels, Belgium
RECRUITINGKatholiek Universiteit Leuven Campus Kortenberg
Leuven, Belgium
RECRUITINGChange in depressive symptom severity (HDRS-17)
Change in severity of depression measured as the change in the 17-point scale of the Hamilton Depression Rating Scale (HDRS-17; score is ranging from 0 to 52, higher scores indicate higher severity of depressive symptoms) between baseline and endpoint
Time frame: T0 -> T6 (12 weeks)
Remission rate of depression (HDRS-17)
Rates of remission measured as a score of ≤7 on the 17-point scale of the Hamilton Depression Rating Scale (HDRS-17; score is ranging from 0 to 52, higher scores indicate higher severity of depressive symptoms and scores 0-7 are considered as being normal) at endpoint
Time frame: T0 -> T6 (12 weeks)
Change in depressive symptom severity (IDS-30SR)
Change in severity of depression measured as the change in the Inventory of Depressive Symptomatology - Self Report (IDS-SR; score is ranging from 0 to 84, higher scores indicate higher severity of depressive symptoms)
Time frame: T0 -> T6 (12 weeks)
Response rate of depressive symptoms (HDRS-17)
Response rates of the depressive symptoms measured on the 17-point scale of the Hamilton Depression Rating Scale (HDRS-17; score is ranging from 0 to 52, higher scores indicate higher severity of depressive symptoms), with response being defined as a 50% reduction in HDRS-17-score from baseline and partial response as a 25% reduction.
Time frame: T0 -> T6 (12 weeks)
Change in night-time sleep (PSQI)
Change in night-time sleep quality and/or quantity measured on the Pittsburgh Sleep Quality Index (PSQI; score is ranging from 0 to 21, higher scores indicate more sleep disturbances)
Time frame: T0 -> T6 (12 weeks)
This platform is for informational purposes only and does not constitute medical advice. Always consult a qualified healthcare professional.
Change in anxiety (STAI)
Change in anxiety measured on the Stait Trait Anxiety Inventory-Self Report (STAI; score is ranging from 20 tot 80, higher scores indicate higher levels of anxiety intensity)
Time frame: T0 -> T6 (12 weeks)
Change in core assessment of psychomotor change (CORE)
Change in the degree of psychomotor disturbance (which is as an integral component of melancholia) measured on the Core Assessment Of Psychomotor Change (CORE; score is ranging from 0-54, higher scores indicate higher levels of psychomotor disturbances)
Time frame: T0 -> T6 (12 weeks)
Depressive symptom profiles (IDS-SR)
Profile of the depression measured on the Inventory of Depressive Symptomatology - Self Report (IDS-SR; score is ranging from 0 to 84, higher scores indicate higher severity of depressive symptoms)
Time frame: T0 -> T6 (12 weeks)
Therapy compliance (MARS)
Therapy compliance measured on the Medication Adherence Scale (MARS; score is ranging from 0-10, higher scores indicate better medication adherence)
Time frame: T0 -> T6 (12 weeks)
Adverse effects
Side effects measured with a questionnaire based on the list as used in the Antidepressant Side-Effect Checklist (ASEC-21) and the known side effects of Minocycline and Celecoxib
Time frame: T0 -> T6 (12 weeks)
Metabolic blood markers
Cholesterol (mg/dl), High Density Lipoprotein (HDL) (mg/dl), Low Density Lipoprotein (LDL) (mg/dl), fasting glucose (mg/dl), triglycerides (mg/dl)
Time frame: T0 -> T6 (12 weeks)
Other metabolic measures
Waist circumference (cm), height (cm) will be measured to calculate the BMI (kg/m\^2)
Time frame: T0 -> T6 (12 weeks)
Other metabolic measures
Weight (kg) will be measured to calculate the BMI (kg/m\^2)
Time frame: T0 -> T6 (12 weeks)