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Trial registered on ANZCTR
Registration number
ACTRN12624000328572
Ethics application status
Approved
Date submitted
5/02/2024
Date registered
25/03/2024
Date last updated
26/08/2024
Date data sharing statement initially provided
25/03/2024
Type of registration
Prospectively registered
Titles & IDs
Public title
Medicinal cannabis for endometriosis: The EndoCann Trial
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Scientific title
A placebo controlled, double blind, randomised controlled trial assessing the effect of medicinal cannabis on pelvic pain in adults with endometriosis: The Endocann trial
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Secondary ID [1]
311296
0
None
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Universal Trial Number (UTN)
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Trial acronym
ENDOCANN
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Linked study record
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Health condition
Health condition(s) or problem(s) studied:
Endometriosis
332534
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Condition category
Condition code
Reproductive Health and Childbirth
329227
329227
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0
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Other reproductive health and childbirth disorders
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Reproductive Health and Childbirth
329813
329813
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0
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Menstruation and menopause
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Alternative and Complementary Medicine
329814
329814
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0
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Other alternative and complementary medicine
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Intervention/exposure
Study type
Interventional
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Description of intervention(s) / exposure
Arm 1: Balanced THC:CBD oil
Participants will first undergo a run-in period (week 0-2) to determine their maximum dosage of interventional product. Participants will start with self-administering 0.40ml of THC:CBD oil (10mg/ml THC: 10mg/ml CBD) per day split into two doses 10-12 hours apart and ingested orally (0.20ml at breakfast and 0.20ml at dinner), providing a total starting dosage of 4mg of THC and CBD per day. This will be increased by 0.20ml per day every two to three days (based on patient preference) until participants report either (a) a 20% or greater reduction in their daily pelvic pain severity as measured on a 0-10 numeric rating scale (NRS), (b) they experience adverse psychoactive effects that are bothersome to the participant, or (c) they reach the maximum dosage of 20mg of THC per day. During the intervention period (week 3-26) participants will continue taking their maximum dosage via self-administration as determined during the run-in period.
Arm 2: Cannabidiol (CBD) full spectrum extract
Participants will first undergo a run-in period (week 0-2) to determine their maximum dosage of interventional product. Participants will start with self-administrating 0.40ml of CBD oil (100mg/ml CBD) per day split into two doses 10-12 hours apart and ingested orally (0.20ml at breakfast and 0.20ml at dinner), providing a total starting dosage of 40mg of CBD per day. This will be increased by 0.20ml per day every two to three days (based on patient preference) until participants report either (a) a 20% or greater reduction in their daily pelvic pain severity as measured on a 0-10 numeric rating scale (NRS), (b) they experience adverse psychoactive effects that are bothersome to the participant, or (c) they reach the maximum dosage of 150mg of CBD per day. During the intervention period (week 3-26) participants will continue taking their maximum dosage via self-administration as determined during the run-in period.
Both Arm 1 and 2 will have an intervention duration of 26 weeks, inclusive of the two-week run-in period.
Compliance will be measured by returning empty bottles twice during the intervention period.
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Intervention code [1]
327742
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Treatment: Drugs
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Comparator / control treatment
Arm 3: Placebo oil: A flavour-matched oil identical to the Arm 1 and Arm 2 interventions. The composition is TGA approved colourant in medium chain triclyceride (MCT) oil + 1% or less terpenes to match the taste of Arm 1 and 2.
Participants will undergo a run-in period (week 0-2) to mimic the dosage schedule of intervention arms. Participants will start with self-administering 0.40ml of placebo oil per day
split into two doses 10-12 hours apart and ingested orally (0.20ml at breakfast and 0.20ml at dinner). This will be increased by 0.20ml per day every two to three days (based on patient preference) until participants report either (a) a 20% or greater reduction in their daily pelvic pain severity as measured on a 0-10 numeric rating scale (NRS), (b) they experience adverse psychoactive effects that are bothersome to the participant, or (c) they reach the maximum consumption of 1.5ml of placebo oil per day. During the intervention period (week 3-26) participants will continue taking their maximum dosage via self-administration as determined during the run-in period.
Arm 3 will have an intervention duration of 26 weeks, inclusive of the two-week run-in period.
Compliance will be measured by returning empty bottles twice during the intervention period.
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Control group
Placebo
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Outcomes
Primary outcome [1]
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Overall pelvic pain severity
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Assessment method [1]
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Pelvic pain severity will be measured on a 100mm VAS.
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Timepoint [1]
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During the run-in period (week 0 – week 3 after trial entry), participants will record their pelvic pain severity daily. A retrospective score of average pelvic pain severity over previous 7 days will be measured weekly during the active intervention period (weekly for 26 weeks after trial entry; the week 13 and week 26 timepoints will be primary timepoints). A retrospective score of average pelvic pain intensity over the previous month will be measured monthly during the follow-up phase (up to week 78 after trial entry; week 52 and week 78 timepoints will be primary timepoints).
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Primary outcome [2]
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Safety outcome #1: Adverse events
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Assessment method [2]
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Adverse events will be assessed in accordance with the Common Terminology Criteria for Adverse Events (CTCAE5.0). Adverse events (e.g., decreased appetite, diarrhoea, drowsiness) will be assessed using a study specific self-report questionnaire that captures intensity (mild, moderate, severe), causality (unrelated, possibly, probably, definitely), severity (grade 1-5), and expectedness (expected, unexpected). All reported adverse events will be followed up by a member of the research team within 48 working hours of being reported.
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Timepoint [2]
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Adverse events will be recorded throughout the entire trial period (78 weeks after trial entry).
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Primary outcome [3]
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Safety outcome #2: Liver and kidney function
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Assessment method [3]
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Blood tests will be performed to assess liver and kidney function. Parameters to be assessed include Liver ALT, ALP, AST, bilirubin, albumin, total protein, GGT, PT, urea, electrolytes (sodium, potassium, chloride, bicarbonate), and full blood count.
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Timepoint [3]
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Safety blood tests will be taken at screening (prior to randomisation), mid-intervention (13 weeks after trial entry), end of intervention (26 weeks after trial entry), and follow-up at week 78 (18 months after trial entry). The primary timepoints are mid-intervention, end of intervention, and follow-up at week 78 after trial entry.
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Secondary outcome [1]
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Most impactful symptom
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Assessment method [1]
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Most impactful symptom (MIS) will be measured by the Most Impactful Symptom Questionnaire (MISQ). Participants will score MIS on a 5-point impact scale, with 1 = not at all and 5 = extremely with a recall period of 3 months. The change in MIS score for each participant will be aggregated across the sample to provide an overall ‘change in MIS score’.
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Timepoint [1]
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Baseline, end of intervention (26 weeks after trial entry), follow-up at week 52 (12 months after trial entry), and follow-up at week 78 (18 months after trial entry)
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Secondary outcome [2]
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Quality of life (QoL) via The Endometriosis Health Profile 30 (EHP-30).
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Assessment method [2]
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The EHP-30 is a user-friendly, validated, and reliable condition-specific tool to assess health-related QoL. The recall period is the previous 4 weeks. Both the main EHP-30 questionnaire and optional modules will be used (where applicable).
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Timepoint [2]
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Baseline, end of intervention (26 weeks after trial entry), follow-up at week 52 (12 months after trial entry), and follow-up at week 78 (18 months after trial entry).
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Secondary outcome [3]
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Depression
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Assessment method [3]
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Depression will be assessed by the Patient-Reported Outcomes Measurement Information System (PROMIS) emotional distress (PED) depression - short form. The PED depression short form is a well-validated, reliable brief measure of depression with excellent internal consistency. The PED is an 8-item measure assessing the cognitive and affective expressions of depression. The individual is asked to rate the severity of symptoms of depressed mood, during the past 7 days, on a 5-point scale
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Timepoint [3]
430517
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Baseline, end of intervention (26 weeks after trial entry), follow-up at week 52 (12 months after trial entry), and follow-up at week 78 (18 months after trial entry).
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Secondary outcome [4]
430518
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Anxiety
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Assessment method [4]
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Anxiety will be assessed by the PROMIS emotional distress - anxiety short form. It is a well-validated, reliable brief measure of anxiety with excellent internal consistency. The PED anxiety short form is 7-item scale measuring anxiety symptoms, encompassing fears, worries, and somatic symptoms. Items are rated on a 5-point scale.
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Timepoint [4]
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Baseline, end of intervention (26 weeks after trial entry), follow-up at week 52 (12 months after trial entry), and follow-up at week 78 (18 months after trial entry)
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Secondary outcome [5]
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Distress
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Assessment method [5]
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Distress will be assessed by the Patient Health Questionnaire (PHQ-15). The PHQ-15 is a valid and reliable tool that measures the distress relating to 15 somatic symptoms (e.g., headaches, dizziness, back pain) that an individual may have experienced over a 7-day period. The PHQ-15 uses a 3-point scale to rate somatic symptom distress.
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Timepoint [5]
430519
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Baseline, end of intervention (26 weeks after trial entry), follow-up at week 52 (12 months after trial entry), and follow-up at week 78 (18 months after trial entry).
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Secondary outcome [6]
430520
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Gastrointestinal symptoms
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Assessment method [6]
430520
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Gastrointestinal symptoms will be measured using the Gastrointestinal Unhelpful Thinking scale (GUTs). The GUTs is a brief 15-item psychometrically valid measure of visceral anxiety and pain catastrophizing. The GUTs assess, in tandem, the primary cognitive-affective drivers of brain-gut dysregulation - gastrointestinal-specific visceral anxiety, and pain catastrophizing. The 15 items will be measured on a 6-point scale.
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Timepoint [6]
430520
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Baseline, end of intervention (26 weeks after trial entry), follow-up at week 52 (12 months after trial entry), and follow-up at week 78 (18 months after trial entry).
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Secondary outcome [7]
430521
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Central sensitisation
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Assessment method [7]
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Central sensitsation will be assessed using the Fibromyalgia Criteria-2016. The Fibromyalgia Criteria-2016 includes 6-items related to symptoms, and a question on pain sites, and is considered to be the gold standard of central sensitisation self-report measures.
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Timepoint [7]
430521
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Baseline, end of intervention (26 weeks after trial entry), follow-up at week 52 (12 months after trial entry), and follow-up at week 78 (18 months after trial entry).
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Secondary outcome [8]
430522
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Analgesic medication usage
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Assessment method [8]
430522
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Analgesic medication usage will be assessed by self-report. The self-report log will capture opioid and non-opioid analgesic medications (e.g., NSAIDs) used to manage pelvic pain symptoms.
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Timepoint [8]
430522
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Analgesic medication usage will be assessed once per week (recalling the previous week) from baseline to end of intervention (week 26 after trial entry) and once per month during the follow-up phase (up to week 78 after trial entry).
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Secondary outcome [9]
430523
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Fatigue
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Assessment method [9]
430523
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Fatigue will be assessed using the PROMIS Fatigue short form. The PROMIS Fatigue short form provides a measure of the experience of fatigue (frequency, duration, and intensity) and the impact of fatigue on physical, mental, and social activities over a 7-day period.
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Timepoint [9]
430523
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Baseline, end of intervention (26 weeks after trial entry), follow-up at week 52 (12 months after trial entry), and follow-up at week 78 (18 months after trial entry).
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Secondary outcome [10]
430524
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Healthcare service usage
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Assessment method [10]
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Healthcare service usage will be assessed using data collected from consenting (opt-in consent) and enrolled participants into the National Endometriosis Clinical and Scientific Trials (NECST) Registry. Participants will be followed to collect data on symptom(s) and/or medication(s) changes/additions.
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Timepoint [10]
430524
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Participants will be followed from baseline to follow-up at week 52 (12 months after trial entry).
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Secondary outcome [11]
430525
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Endometriosis lesion progression and staging
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Assessment method [11]
430525
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Endometriosis lesion progression and staging will be assessed together as a composite secondary outcome using transvaginal ultrasound (tVUS). Evaluation for endometriosis will primarily follow the published consensus approach by the International Deep Endometriosis Analysis (IDEA) group. . Each individual endometriosis deposit will be characterised as superficial, deep or ovarian. In the case of ovarian and deep endometriosis, deposits will be measured in three orthogonal planes. The #Enzian system will be used to determine endometriosis staging.
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Timepoint [11]
430525
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All participants will have a tVUS at baseline prior to beginning the intervention. A sub-set of 45 participants (15 each arm) will have two more scans, one at end of intervention (26 weeks after trial entry) and follow-up at 78 weeks (18 months after trial entry).
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Secondary outcome [12]
430528
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Inflammatory plasma markers
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Assessment method [12]
430528
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Inflammatory markers will be assessed via blood samples. Inflammatory markers assessed include: interleukin-6 and tumour necriosis factor-a.
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Timepoint [12]
430528
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Blood samples will be taken at screening (before randomisation), mid-intervention (13 weeks after trial entry), end of intervention (26 weeks after trial entry), and follow-up at 78 weeks (18 months after trial entry).
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Secondary outcome [13]
432414
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QoL via the European Quality of Life Five Dimension (EQ-5D-5L).
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Assessment method [13]
432414
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The EQ-5D-5L is a reliable and valid generic health-related QoL questionnaire, which measures five domains, including mobility, self-care, usual activities, pain/discomfort, and anxiety/depression. Each dimension has 5 levels: no problems (Level 1), slight problems, moderate problems, severe problems, and extreme problems (Level 5). The EQ-5D-5L also includes a visual rating scale, where the respondent is asked to rate how good or bad their health is at that moment in time, with 0 = Worst Health Imaginable and 100 = Best Health Imaginable.
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Timepoint [13]
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Baseline, end of intervention (26 weeks after trial entry), follow-up at week 52 (12 months after trial entry), and follow-up at week 78 (18 months after trial entry).
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Secondary outcome [14]
432415
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Presence of irritable bowel syndrome (IBS)
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Assessment method [14]
432415
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The presence of IBS will be measured by a 5-item questionnaire based on the Rome IV criteria. Each item will be answered using a yes or no response.
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Timepoint [14]
432415
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Baseline, end of intervention (26 weeks after trial entry), follow-up at week 52 (12 months after trial entry), and follow-up at week 78 (18 months after trial entry).
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Secondary outcome [15]
432416
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IBS Severity
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Assessment method [15]
432416
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IBS severity will be measured using the IBS-severity scale (IBS-SS). The IBS-SS is part one of the IBS Questionnaire. The IBS-SS consists of four parts with seven sub-items that measure IBS severity. Apart from pain frequency, all questions are answered by using a 0 –100 VAS.
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Timepoint [15]
432416
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Baseline, end of intervention (26 weeks after trial entry), follow-up at week 52 (12 months after trial entry), and follow-up at week 78 (18 months after trial entry).
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Secondary outcome [16]
432417
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Subjective cognitive functioning via the Ecological momentary assessment.
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Assessment method [16]
432417
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The EMA will involve participants answering a single question (How much change have you noticed in your memory and concentration since you started this trial’?).
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Timepoint [16]
432417
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Participants will log their responses daily during the run-in period (up to week 3 after trial entry), and then weekly until end of intervention (week 26 after trial entry), and thereafter monthly to end of follow up at week 78 (18 months after trial entry).
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Secondary outcome [17]
432418
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Subjective cognitive functioning via and the Functional Assessment of Cancer Therapy—Cognition (FACT-Cog) scale.
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Assessment method [17]
432418
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The FACT-Cog scale is a 37-item scale designed to assess cognitive functioning and cognitive difficulties.
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Timepoint [17]
432418
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Baseline, end of intervention (26 weeks after trial entry), follow-up at week 52 (12 months after trial entry), and follow-up at week 78 (18 months after trial entry).
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Secondary outcome [18]
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Objective cognitive functioning via the Symbol Digit Modalities Test
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Assessment method [18]
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A subset of participants (n=60; 20 participants per trial arm) will undergo further objective cognitive functioning assessment via the Symbol Digit Modalities Test - Oral version. It is a commonly used test of psychomotor speed, which measures processing speed and motor speed.
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Timepoint [18]
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Baseline, end of intervention (26 weeks after trial entry), and follow-up at week 52 (12 months after trial entry).
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Secondary outcome [19]
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Objective cognitive functioning via the Digit Span (Forward and Backward).
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Assessment method [19]
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A subset of participants (n=60; 20 participants per trial arm) will undergo further objective cognitive functioning assessment via the Digit Span (Forward and Backward) (from the Wechsler Adult Intelligence Scale- Fourth Edition (WAIS-IV)), is a measure of working memory.
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Timepoint [19]
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Baseline, end of intervention (26 weeks after trial entry), and follow-up at week 52 (12 months after trial entry).
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Secondary outcome [20]
432421
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Objective cognitive functioning via The Rey Auditory Verbal Learning Test (RAVLT).
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Assessment method [20]
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A subset of participants (n=60; 20 participants per trial arm) will undergo further objective cognitive functioning assessment via the Rey Auditory Verbal Learning Test (RAVLT). RAVLT measures verbal memory. It involves participants listening to a list of 15 nouns and then being asked to recall as many words as possible from the list. This is then repeated after a 20-minute delay.
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Timepoint [20]
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Baseline, end of intervention (26 weeks after trial entry), and follow-up at week 52 (12 months after trial entry).
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Secondary outcome [21]
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Objective cognitive functioning via the Delis-Kaplan Executive Function System (D-KEFS) test.
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Assessment method [21]
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A subset of participants (n=60; 20 participants per trial arm) will undergo further objective cognitive functioning assessment via the Delis-Kaplan Executive Function System (D-KEFS) test.
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Timepoint [21]
432422
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Baseline, end of intervention (26 weeks after trial entry), and follow-up at week 52 (12 months after trial entry).
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Secondary outcome [22]
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Sleep quality
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Assessment method [22]
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Subjective sleep quality will be assessed by the Athens Insomnia Inventory (AIS), a validated and reliable brief 8-item self-report measure.
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Timepoint [22]
432423
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Baseline, end of intervention (26 weeks after trial entry), and follow-up at week 52 (12 months after trial entry).
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Secondary outcome [23]
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Cannabinoid plasma markers
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Assessment method [23]
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Cannabinoid and markers will be assessed via blood samples. Cannabinoid markers to be assessed include: Cannabidiol, THC, Anandamide, 1-Arachidonoylglycerol, 2-Arachidonoylglycerol, Palmitoylethanolamide, Stearoylethanolamide, oleoylethanolamide.
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Timepoint [23]
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Blood samples will be taken at screening (before randomisation), mid-intervention (13 weeks after trial entry), end of intervention (26 weeks after trial entry), and follow-up at 78 weeks (18 months after trial entry).
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Eligibility
Key inclusion criteria
- Aged over 18 years.
- Self-reported pelvic pain, severe enough to seek medical attention.
- Diagnosis of endometriosis via laparoscopy (with or without histological confirmation), magnetic resonance imaging (MRI), or Ultrasound imaging by a medical doctor, with input from an imaging specialist with specific endometriosis expertise.
- Have not used illicit cannabis and/or prescribed cannabinoid-based medications in the previous three months.
- Report no current, or history of, hazardous cannabis use, or dependency.
- If sexually active and pregnancy is a possibility, agree to use appropriate contraception to prevent pregnancy during the study period.
- Agree to keep all study product stored in a secure location and not to share/distribute cannabis to any other individual.
- Agree not to drive while under the effects of medicinal cannabis.
- Willing to provide informed consent and adhere to the protocol.
- Residing in New South Wales during the trial period.
- Able to travel to NICM Health Research Institute, The Royal Hospital for Women, Sydney Endometriosis, and Macquarie University for data collection.
- Able to travel to a Laverty collection centre for blood tests.
- Has internet access (either via a mobile (Apple or Android) or tablet (Apple)) for logging outcomes via the OnTracka app.
- Ability to understand and speak English.
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Minimum age
18
Years
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Maximum age
No limit
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Sex
Females
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Can healthy volunteers participate?
No
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Key exclusion criteria
- Have had endometriosis-related surgery in the previous six months or have any surgery planned during the study period.
- Started, stopped, or had a significant change in dosage of any endometriosis specific medication in the last three months. This includes contraceptives, GNRH-a, and neuroleptics (changes in ‘as needed’ medications such as analgesics are not reasons for exclusion).
- Have any current or past diagnoses that would be considered a risk to participation in the study, including but not limited to, schizophrenia spectrum and other psychotic disorders, bipolar-related disorders, dissociative disorders, personality disorders, cannabis use disorder, obsessive-compulsive related disorders, neurological disorders, or brain injury.
- Currently have any major haematological, endocrine, cerebrovascular, cardiovascular, coronary, pulmonary, gastrointestinal (particularly hepatic), renal, or neurological disease (determined by the medical monitoring team).
- Current usage of anticoagulants (e.g., warfarin, heparin or any other NOAC/DOAC medications) or any other medication, including supplements (e.g., vitamin E, Gingko), that causes blood thinning.
- Currently pregnant or breastfeeding or planning on becoming pregnant during the study period.
- Abnormal liver and kidney function tests as determined during screening process.
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Study design
Purpose of the study
Treatment
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Allocation to intervention
Randomised controlled trial
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Procedure for enrolling a subject and allocating the treatment (allocation concealment procedures)
Central randomisation will be performed by a clinical trials manager who is external to the study using REDCap's randomisation function. Allocation is concealed by this software so that none of the research team has access to this.
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Methods used to generate the sequence in which subjects will be randomised (sequence generation)
Simple randomisation will be perfomed by REDCap's randomisation function. Participants will be randomised in a 1:1:1 ratio.
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Masking / blinding
Blinded (masking used)
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Who is / are masked / blinded?
The people receiving the treatment/s
The people assessing the outcomes
The people analysing the results/data
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Intervention assignment
Parallel
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Other design features
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Phase
Phase 2 / Phase 3
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Type of endpoint/s
Safety/efficacy
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Statistical methods / analysis
Based on a minimum clinically important difference (MCID) of 20mm for pelvic pain severity, in line with both clinical expert opinion and the IMMPACT recommendations for chronic pain, and a standard deviation (SD) of 22.7 for the change in VAS, 90% power, and a two-sided alpha of 5%, each treatment group would require 29 participants. Accounting for an assumed dropout rate of 30%, 42 participants would be required per arm, with 126 total.
All analyses (excluding safety) will be by intention-to treat using the full analysis set. The primary outcome will also be analysed secondarily using the per protocol set. The safety analysis set will be used for all safety analyses. All estimates will be given as 95% confidence intervals, and so with a nominal two-sided type I error rate of 5%.
Data description will be by count and proportion expressed as percentage for categorical variables, and by mean and standard deviation (SD), inter-quartile range (IQR), and min to max as range for continuous variables.
Primary endpoint analysis (pelvic pain severity):
The primary analysis will be by general linear model (ANCOVA) with baseline pelvic pain severity score as a continuous covariate.
The pre-specified treatment comparisons (Intention to treat (ITT) and per-protocol (PP)) are:
- Arm 1 compared to placebo,
- Arm 2 compared to placebo, and
- Arm 1 compared to Arm 2.
Secondary end-point analyses:
The pre-specified treatment comparisons (Intention to treat (ITT) and per-protocol (PP)) are as specified for primary endpoint analysis.
The following methods will be used:
1) Simple t-test by time of measurement and mixed linear models for repeated measures by time:
- Change in most bothersome symptom score
- Quality of life
- Changes in analgesic medication usage
- Psychological measures (depression, anxiety, distress)
- Fatigue
- Gut measures
- Central sensitization
- Subjective cognitive functioning
2) Comparison of proportions by logistic regression:
- Adverse Events
- Serious Adverse Events
- Related Adverse Events.
Sub-group analyses:
Subgroup analyses of the primary endpoint will be made to assess the consistency of the intervention effect across the following subgroups:
- Pelvic pain severity at baseline: moderate/severe pain vs no/mild pain
- Stage of endometriosis
- Bodyweight
- Age.
If the number of participants is too small (less than 10%) within a subgroup, then the subgroup categories may be redefined prior to unblinding the study.
Other analyses:
1) Endocannabinoid and inflammatory markers
The cannabinoids and inflammatory markers will be quantified in NICMs TGA licenced analytical and PCS pharmacology laboratory. Plasma levels (in pmol/ml) of major cannabinoids (CBD, THC), related metabolites of CBD and THC (AEA, 1-AG, 2-AG, PEA, SEA and OEA), and inflammatory markers (IL-6, TNFa) will be compared to pelvic pain severity score at four time points: baseline, mid-intervention (week 13), end of intervention (week 26), and post-intervention follow-up 2 (week 78). Statistical analysis between the treatment arms in Study 1 and endocannabinoid levels will be via a linear mixed model with time and group as fixed effects. The relationship between each of the four endocannabinoids and pelvic pain intensity will be assessed using either linear or ordinal regression depending on the normality of data.
2) Endometriosis lesion progression and staging
Endometriosis lesion change will be compared in the sub-set of participants who consent to undertake undergo repeat scans over the course of the study. Disease presence by anatomical site, and stage as per #Enzian (which includes presence/absence of adenomyosis) will be used as factors in the main statistical analysis to determine if they are related to response/non-response to treatment. Although it remains unknown what metric may be the most valuable in assessing interval change (e.g. single measurement (e.g. length) versus volume), the study experts have determined a priori that a change in lesion size over time of >10% will be considered significant.
For superficial endometriosis, the size of lesions is almost negligible so assessing change will not be possible. However, we will attempt to document a change in the presence of lesions from scan to scan, but only if there is consistently sufficient fluid to assess a region. For example, if superficial endometriosis is noted on the uterosacral ligament on one scan, aided by the presence of free fluid, but no free fluid is present at the next scan, the repeat assessment will be considered incomplete for superficial endometriosis.
3) Healthcare utilisation
All data will be analysed and presented as de-identified, grouped data. Descriptive statistics such as means, standard deviations, medians, inter-quartile ranges (for the continuous variables) and frequency (for the categorical variables) will be used. Cross tabulations and relevant statistical tests (e.g., chi squared) may be performed to describe demographic characteristics associated with an endometriosis patient diagnosis, acquisition of surgical and/or medical management.
No small cell sizes will be published where they could result in the possible identification of a participant e.g., using postcode level data against key characteristics. Geographical data and related classifications will use area levels appropriate to the number of participants e.g., state, Accessibility/Remoteness Index of Australia (ARIA), Socio-Economic Indexes for Areas (SEIFA), groupings larger than postcode to prevent small cell sizes arising. No individual level data that could identify non-participants e.g., family members will be reported.
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Recruitment
Recruitment status
Recruiting
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Date of first participant enrolment
Anticipated
11/04/2024
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Actual
11/04/2024
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Date of last participant enrolment
Anticipated
1/07/2025
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Actual
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Date of last data collection
Anticipated
1/07/2026
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Actual
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Sample size
Target
126
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Accrual to date
2
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Final
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Recruitment in Australia
Recruitment state(s)
NSW
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Funding & Sponsors
Funding source category [1]
315550
0
Charities/Societies/Foundations
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Name [1]
315550
0
The Wilson Foundation
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Address [1]
315550
0
GPO Box 4658, Sydney NSW 2001
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Country [1]
315550
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Australia
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Primary sponsor type
University
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Name
Western Sydney University
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Address
GPO Box 4658, Sydney NSW 2001
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Country
Australia
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Secondary sponsor category [1]
317638
0
Charities/Societies/Foundations
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Name [1]
317638
0
The Wilson Foundation
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Address [1]
317638
0
NICM Health Research Institute, Western Sydney University, Locked Bag 1797, Penrith NSW 2751
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Country [1]
317638
0
Australia
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Ethics approval
Ethics application status
Approved
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Ethics committee name [1]
314449
0
Western Sydney University Human Research Ethics Committee
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Ethics committee address [1]
314449
0
Western Sydney University, Werrington South Campus, Locked Bag 1797 PENRITH NSW 2751
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Ethics committee country [1]
314449
0
Australia
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Date submitted for ethics approval [1]
314449
0
06/11/2023
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Approval date [1]
314449
0
05/03/2024
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Ethics approval number [1]
314449
0
H15755
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Summary
Brief summary
Endometriosis is an oestrogen-dependent, chronic inflammatory condition characterised by the presence of endometrial-like tissue outside of the uterus in the form of lesions, affecting around 1 in 7 women and those assigned female at birth in Australia. Endometriosis has a significant impact on one's physical, psychological, and social wellbeing. Unfortunately many of the pharmaceutical medications for endometriosis have bothersome side effects or should only be used for a short period of time due to concerns related to dependence and addiction. Medicinal cannabis has well described analgesic, anti-inflammatory, anxiolytic, anti-depressant, and anti-emetic actions. Cannabis use in other chronic pain conditions has resulted in “substitution” of pharmaceuticals, commonly opioid analgesics, for cannabis. Our previous research has shown that women with endometriosis in Australia are using mostly illicit sources of cannabis to manage their pain and other symptoms. We hypothesise that either a balanced THC:CBD oil or CBD alone will reduce pelvic pain and other symptoms in women with endometriosis. The primary aim of this study is to determine the efficacy and safety of two medicinal cannabis products compared to placebo in women with endometriosis.
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Trial website
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Trial related presentations / publications
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Public notes
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Contacts
Principal investigator
Name
131622
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A/Prof Mike Armour
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Address
131622
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NICM Health Research Institute, Western Sydney University, Building J, Westmead Campus, Locked Bag 1797, PENRITH NSW 2751
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Country
131622
0
Australia
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Phone
131622
0
+61296854720
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Fax
131622
0
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Email
131622
0
[email protected]
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Contact person for public queries
Name
131623
0
Mike Armour
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Address
131623
0
NICM Health Research Institute, Western Sydney University, Building J, Westmead Campus, Locked Bag 1797, PENRITH NSW 2751
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Country
131623
0
Australia
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Phone
131623
0
+61296854720
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Fax
131623
0
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Email
131623
0
[email protected]
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Contact person for scientific queries
Name
131624
0
Mike Armour
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Address
131624
0
NICM Health Research Institute, Western Sydney University, Building J, Westmead Campus, Locked Bag 1797, PENRITH NSW 2751
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Country
131624
0
Australia
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Phone
131624
0
+61296854720
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Fax
131624
0
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Email
131624
0
[email protected]
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Data sharing statement
Will individual participant data (IPD) for this trial be available (including data dictionaries)?
No
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No/undecided IPD sharing reason/comment
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What supporting documents are/will be available?
No Supporting Document Provided
Results publications and other study-related documents
Documents added manually
No documents have been uploaded by study researchers.
Documents added automatically
No additional documents have been identified.
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