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The Effect of Pain Neuroscience Education and Behavioural Graded Activity on Chronic Pain in Breast Cancer Survivors (BCS-PAIN)

Primary Purpose

Breast Neoplasms, Survivors, Chronic Pain

Status
Recruiting
Phase
Not Applicable
Locations
Belgium
Study Type
Interventional
Intervention
Pain Neuroscience Education
Behavioural Graded Activity
Usual care
Sponsored by
Universitair Ziekenhuis Brussel
About
Eligibility
Locations
Arms
Outcomes
Full info

About this trial

This is an interventional treatment trial for Breast Neoplasms focused on measuring Behavioural Graded Activity, Pain Neuroscience Education

Eligibility Criteria

18 Years - undefined (Adult, Older Adult)FemaleDoes not accept healthy volunteers

Inclusion Criteria:

  • To meet the definition introduced by the National Cancer Institute's Office of Cancer Survivorship, in which a cancer survivor is a patient with a history of cancer that is beyond the acute diagnosis and treatment phase. Patients need to be cancer-free and should have finished their primary treatment with a curative intent for at least 3 months prior to study participation. Adjuvant hormonal therapy and immunotherapy form the exception to the rule and are tolerated.
  • To report a pain severity of at least 3 out of 10 on pain visual analogue scale.
  • To be able to speak and read in Dutch in order to give informed consent and to complete the assessment tools. Written and signed consent will be obtained from all participants.

Exclusion Criteria:

  • Suffering from dementia or cognitive impairment (unable to understand the test instructions and/or Mini Mental State Examination score <23/30).
  • Suffering from severe psychological or psychiatric diseases.
  • Diagnosis of new neoplasms or metastases.

Sites / Locations

  • Vrije Universiteit Brussel (VUB)Recruiting

Arms of the Study

Arm 1

Arm 2

Arm Type

Experimental

Active Comparator

Arm Label

Pain Neuroscience Education + Behavioural Graded Activity

Usual care

Arm Description

Patients allocated to the intervention group will receive a 12-week treatment program that consists of 6 sessions, in which 'Pain Neuroscience Education' and 'Behavioural Graded Activity' will be integrated.

Patients allocated to the control group will receive an information leaflet from "Kom op tegen kanker" regarding "Pain in and after cancer".

Outcomes

Primary Outcome Measures

Change in pain intensity and pain interference
Change between baseline (T1) and 3 months post-intervention (T3) Measured with the 'Brief Pain Inventory' The minimum and maximum values: 0, 10 Higher score means a worse outcome
Self-reported pain intensity and pain interference
Measured with the 'Brief Pain Inventory' The minimum and maximum values: 0, 10 Higher score means a worse outcome
Self-reported pain intensity and pain interference
Measured with the 'Brief Pain Inventory' The minimum and maximum values: 0, 10 Higher score means a worse outcome
Self-reported pain intensity and pain interference
Measured with the 'Brief Pain Inventory' The minimum and maximum values: 0, 10 Higher score means a worse outcome
Self-reported pain intensity and pain interference
Measured with the 'Brief Pain Inventory' The minimum and maximum values: 0, 10 Higher score means a worse outcome
Self-reported pain intensity and pain interference
Measured with the 'Brief Pain Inventory' The minimum and maximum values: 0, 10 Higher score means a worse outcome

Secondary Outcome Measures

Self-reported health-related quality of life
Measured with the 'European Organisation for Research and Treatment of Cancer Core Quality of Life Questionnaire (EORTC-QLQ-C30)' The minimum and maximum values: 0, 100 Higher score means a better outcome
Temperature detection threshold
Assessed by the Medoc TSA-II Neurosensory Analyzer.
Pain detection threshold
Assessed by the digital algometer, the Medoc TSA-II Neurosensory Analyzer and a manual blood pressure cuff.
Pain tolerance threshold
Assessed by a manual blood pressure cuff.
Endogenous pain inhibition
Assessed objectively by conditioned pain modulation paradigm. A manual blood pressure is the conditioned stimulus, and the digital algometer and the Medoc TSA-II Neurosensory Analyzer are testing stimuli.
Endogenous pain facilitation
Assessed objectively by temporal summation paradigm. Ten testing stimuli will be applied, and subjects will be asked to rate their pain intensity on the first, fifth and tenth stimulus by using the Visual Analogue Scale.

Full Information

First Posted
August 18, 2020
Last Updated
November 4, 2022
Sponsor
Universitair Ziekenhuis Brussel
Collaborators
Fund for Scientific Research, Flanders, Belgium, Vrije Universiteit Brussel
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1. Study Identification

Unique Protocol Identification Number
NCT04531917
Brief Title
The Effect of Pain Neuroscience Education and Behavioural Graded Activity on Chronic Pain in Breast Cancer Survivors
Acronym
BCS-PAIN
Official Title
The Effect of Pain Neuroscience Education and Behavioural Graded Activity Compared to Usual Care on Chronic Pain in Breast Cancer Survivors: a Randomised Controlled Trial
Study Type
Interventional

2. Study Status

Record Verification Date
November 2022
Overall Recruitment Status
Recruiting
Study Start Date
October 12, 2020 (Actual)
Primary Completion Date
April 2024 (Anticipated)
Study Completion Date
April 2024 (Anticipated)

3. Sponsor/Collaborators

Responsible Party, by Official Title
Sponsor
Name of the Sponsor
Universitair Ziekenhuis Brussel
Collaborators
Fund for Scientific Research, Flanders, Belgium, Vrije Universiteit Brussel

4. Oversight

Studies a U.S. FDA-regulated Drug Product
No
Studies a U.S. FDA-regulated Device Product
No

5. Study Description

Brief Summary
Chronic pain in breast cancer survivors (BCS) is of considerable concern as it impacts the health-related quality of life (HRQoL) and activities of daily living negatively. Over the past decades, awareness has raised the value of pain neuroscience education (PNE) in chronic pain. However, pain education remains underused in oncology and is often restricted to a biomedical management, which falls short in explaining persistent pain following cancer. Since PNE alone has rather small effect sizes, it should ideally be combined with a physical part, 'behavioural graded activity' (BGA). Therefore, the purpose of this study is to investigate the effectiveness of PNE with BGA compared to usual care on chronic pain in BCS. A multi-centre, parallel, two-arm, double-blinded superiority with a three months intervention and two years follow-up will be conducted in 200 BCS with chronic pain. These will be randomly assigned to the intervention or usual care group. The intervention group will receive 6 sessions, in which PNE and BGA will be integrated. Whereas, the usual care group will receive an information leaflet regarding "Pain in and after cancer". The primary objective of the present study is to examine whether the combination of PNE and BGA has an added value in decreasing the pain intensity compared to the usual care in BCS with chronic pain. The secondary objectives are to investigate whether the combination of PNE and BGA has the ability to reduce endogenous hyperalgesia and improve HRQoL compared to the usual care in BCS with chronic pain.

6. Conditions and Keywords

Primary Disease or Condition Being Studied in the Trial, or the Focus of the Study
Breast Neoplasms, Survivors, Chronic Pain
Keywords
Behavioural Graded Activity, Pain Neuroscience Education

7. Study Design

Primary Purpose
Treatment
Study Phase
Not Applicable
Interventional Study Model
Parallel Assignment
Masking
InvestigatorOutcomes Assessor
Allocation
Randomized
Enrollment
200 (Anticipated)

8. Arms, Groups, and Interventions

Arm Title
Pain Neuroscience Education + Behavioural Graded Activity
Arm Type
Experimental
Arm Description
Patients allocated to the intervention group will receive a 12-week treatment program that consists of 6 sessions, in which 'Pain Neuroscience Education' and 'Behavioural Graded Activity' will be integrated.
Arm Title
Usual care
Arm Type
Active Comparator
Arm Description
Patients allocated to the control group will receive an information leaflet from "Kom op tegen kanker" regarding "Pain in and after cancer".
Intervention Type
Other
Intervention Name(s)
Pain Neuroscience Education
Intervention Description
Pain Neuroscience Education (PNE) teaches patients about complex pain mechanisms known to be of importance in pain following breast cancer such as malfunctioning of the endogenous analgesic system and pain memories.
Intervention Type
Other
Intervention Name(s)
Behavioural Graded Activity
Intervention Description
Patients in the experimental group will receive a behavioural treatment integrated within the concepts of operant conditioning. The purpose of Behavioural Graded Activity (BGA) is to increase the level of physical activity in the patient's daily lives in a time-contingent manner. On top of that, a healthy behaviour will be positively reinforced to consequently create a withdrawal of the attention towards pain behaviour, which is seen as an unreliable "alarm sign" in chronic pain patients. The implementation of BGA after PNE is described in the guideline reported by the International Association for the Study of Pain.
Intervention Type
Other
Intervention Name(s)
Usual care
Intervention Description
The content of the leaflet has a biomedical approach in explaining pain and providing information on the different pain medication classes. This leaflet is mostly available in waiting rooms of oncology centres and units of the Flemish part of Belgium.
Primary Outcome Measure Information:
Title
Change in pain intensity and pain interference
Description
Change between baseline (T1) and 3 months post-intervention (T3) Measured with the 'Brief Pain Inventory' The minimum and maximum values: 0, 10 Higher score means a worse outcome
Time Frame
T1: baseline (within one week before randomisation) and T3: 3 months after intervention (w 26)
Title
Self-reported pain intensity and pain interference
Description
Measured with the 'Brief Pain Inventory' The minimum and maximum values: 0, 10 Higher score means a worse outcome
Time Frame
T1: baseline (within one week before randomisation)
Title
Self-reported pain intensity and pain interference
Description
Measured with the 'Brief Pain Inventory' The minimum and maximum values: 0, 10 Higher score means a worse outcome
Time Frame
T2: after finishing intervention (week 13)
Title
Self-reported pain intensity and pain interference
Description
Measured with the 'Brief Pain Inventory' The minimum and maximum values: 0, 10 Higher score means a worse outcome
Time Frame
T3: 3 months after intervention (week 26)
Title
Self-reported pain intensity and pain interference
Description
Measured with the 'Brief Pain Inventory' The minimum and maximum values: 0, 10 Higher score means a worse outcome
Time Frame
T4: 1 year after intervention (week 64)
Title
Self-reported pain intensity and pain interference
Description
Measured with the 'Brief Pain Inventory' The minimum and maximum values: 0, 10 Higher score means a worse outcome
Time Frame
T5: 2 years after intervention (week 116)
Secondary Outcome Measure Information:
Title
Self-reported health-related quality of life
Description
Measured with the 'European Organisation for Research and Treatment of Cancer Core Quality of Life Questionnaire (EORTC-QLQ-C30)' The minimum and maximum values: 0, 100 Higher score means a better outcome
Time Frame
T1: baseline (within one week before randomisation), T2: after finishing intervention (w 13), T3: 3 months after intervention (w 26), T4: 1 year after intervention (w 64) and T5: 2 years after intervention (w 116)
Title
Temperature detection threshold
Description
Assessed by the Medoc TSA-II Neurosensory Analyzer.
Time Frame
T1: baseline (within one week before randomisation), T2: after finishing intervention (w 13) and T3: 3 months after intervention (w 26)
Title
Pain detection threshold
Description
Assessed by the digital algometer, the Medoc TSA-II Neurosensory Analyzer and a manual blood pressure cuff.
Time Frame
T1: baseline (within one week before randomisation), T2: after finishing intervention (w 13) and T3: 3 months after intervention (w 26)
Title
Pain tolerance threshold
Description
Assessed by a manual blood pressure cuff.
Time Frame
T1: baseline (within one week before randomisation), T2: after finishing intervention (w 13) and T3: 3 months after intervention (w 26)
Title
Endogenous pain inhibition
Description
Assessed objectively by conditioned pain modulation paradigm. A manual blood pressure is the conditioned stimulus, and the digital algometer and the Medoc TSA-II Neurosensory Analyzer are testing stimuli.
Time Frame
T1: baseline (within one week before randomisation), T2: after finishing intervention (w 13) and T3: 3 months after intervention (w 26)
Title
Endogenous pain facilitation
Description
Assessed objectively by temporal summation paradigm. Ten testing stimuli will be applied, and subjects will be asked to rate their pain intensity on the first, fifth and tenth stimulus by using the Visual Analogue Scale.
Time Frame
T1: baseline (within one week before randomisation), T2: after finishing intervention (w 13) and T3: 3 months after intervention (w 26)
Other Pre-specified Outcome Measures:
Title
Self-reported pain
Description
Measured with the 'Visual Analogue Scale' The minimum and maximum values: 0mm, 100mm Higher score means a worse outcome
Time Frame
T1: baseline (within one week before randomisation), T2: after finishing intervention (w 13), T3: 3 months after intervention (w 26), T4: 1 year after intervention (w 64) and T5: 2 years after intervention (w 116)
Title
Self-reported neuropathic pain
Description
Measured with the 'Douleur Neuropatique 4' The minimum and maximum values: 0, 10 Higher score means a worse outcome A score of 4 or higher indicates neuropathic pain
Time Frame
T1: baseline (within one week before randomisation), T2: after finishing intervention (w 13), T3: 3 months after intervention (w 26), T4: 1 year after intervention (w 64) and T5: 2 years after intervention (w 116)
Title
Self-reported central sensitization
Description
Measured with the 'Central Sensitization Index' The minimum and maximum values: 0, 100 Higher score means a worse outcome A score of 40 or higher indicates the presence of central sensitization
Time Frame
T1: baseline (within one week before randomisation), T2: after finishing intervention (w 13), T3: 3 months after intervention (w 26), T4: 1 year after intervention (w 64) and T5: 2 years after intervention (w 116)
Title
Self-reported physical activity level
Description
Measured with the 'International Physical Activity Questionnaire short form' Total physical activity in MET-min/week and time spent sitting
Time Frame
T1: baseline (within one week before randomisation), T2: after finishing intervention (w 13), T3: 3 months after intervention (w 26), T4: 1 year after intervention (w 64) and T5: 2 years after intervention (w 116)
Title
Self-reported physical activity level
Description
Measured with the 'logbook' Subjects enrolled in the intervention arm will have to fill in the logbook on daily basis.
Time Frame
During the intervention and T2: after finishing intervention (w 13)
Title
Self-reported sleep quality
Description
Measured with the 'Pittsburgh Sleep Quality Index' The minimum and maximum values: 0, 21 Higher score means a worse outcome A scores above 5 indicates poor global sleep quality
Time Frame
T1: baseline (within one week before randomisation), T2: after finishing intervention (w 13), T3: 3 months after intervention (w 26), T4: 1 year after intervention (w 64) and T5: 2 years after intervention (w 116)
Title
Self-reported insomnia severity
Description
Measured with the 'Insomnia Severity Index' The minimum and maximum values: 0, 28 Higher score means a worse outcome A scores of 8 or higher indicates insomnia
Time Frame
T1: baseline (within one week before randomisation), T2: after finishing intervention (w 13), T3: 3 months after intervention (w 26), T4: 1 year after intervention (w 64) and T5: 2 years after intervention (w 116)
Title
Self-reported fatigue
Description
Measured with the 'Fatigue Severity Scale' The minimum and maximum values: 9, 63 Higher score means a worse outcome
Time Frame
T1: baseline (within one week before randomisation), T2: after finishing intervention (w 13), T3: 3 months after intervention (w 26), T4: 1 year after intervention (w 64) and T5: 2 years after intervention (w 116)
Title
Self-reported pain cognitions (pain catastrophizing)
Description
Measured with the 'Pain Catastrophizing Scale' The minimum and maximum values: 0, 52 Higher score means a worse outcome A scores of 30 or higher indicates pain catastrophizing thoughts
Time Frame
T1: baseline (within one week before randomisation), T2: after finishing intervention (w 13), T3: 3 months after intervention (w 26), T4: 1 year after intervention (w 64) and T5: 2 years after intervention (w 116)
Title
Self-reported pain cognitions (perceived injustice)
Description
Measured with the 'Injustice Experience Questionnaire' The minimum and maximum values: 0, 48 Higher score means a worse outcome
Time Frame
T1: baseline (within one week before randomisation), T2: after finishing intervention (w 13), T3: 3 months after intervention (w 26), T4: 1 year after intervention (w 64) and T5: 2 years after intervention (w 116)
Title
Self-reported pain cognitions (illness perception)
Description
Measured with the 'the Brief Illness Perception Questionnaire' The minimum and maximum values: 0, 10 Higher score means a worse outcome
Time Frame
T1: baseline (within one week before randomisation), T2: after finishing intervention (w 13), T3: 3 months after intervention (w 26), T4: 1 year after intervention (w 64) and T5: 2 years after intervention (w 116)
Title
Self-reported pain cognitions (pain vigilance and awareness)
Description
Measured with the 'Pain Vigilance and Awareness questionnaire' The minimum and maximum values: 0, 90 Higher score means a worse outcome
Time Frame
T1: baseline (within one week before randomisation), T2: after finishing intervention (w 13), T3: 3 months after intervention (w 26), T4: 1 year after intervention (w 64) and T5: 2 years after intervention (w 116)
Title
Self-reported depression
Description
Measured with the 'Depression, Anxiety, Stress Scale' The minimum and maximum values: 0, 21 Higher score means a worse outcome
Time Frame
T1: baseline (within one week before randomisation), T2: after finishing intervention (w 13), T3: 3 months after intervention (w 26), T4: 1 year after intervention (w 64) and T5: 2 years after intervention (w 116)
Title
Self-reported anxiety
Description
Measured with the 'Depression, Anxiety, Stress Scale' The minimum and maximum values: 0, 21 Higher score means a worse outcome
Time Frame
T1: baseline (within one week before randomisation), T2: after finishing intervention (w 13), T3: 3 months after intervention (w 26), T4: 1 year after intervention (w 64) and T5: 2 years after intervention (w 116)
Title
Self-reported stress
Description
Measured with the 'Depression, Anxiety, Stress Scale' The minimum and maximum values: 0, 21 Higher score means a worse outcome
Time Frame
T1: baseline (within one week before randomisation), T2: after finishing intervention (w 13), T3: 3 months after intervention (w 26), T4: 1 year after intervention (w 64) and T5: 2 years after intervention (w 116)
Title
Treatment adherence
Description
Patient adherence for the treatment sessions will be calculated as the ratio of the number of treatment sessions that were actually carried out versus the number of prescribed sessions.
Time Frame
During the intervention and T2: after finishing intervention (w 13)
Title
Treatment compliance
Description
Compliance will be calculated as the ratio of the total training duration (recorded in the logbooks) versus the prescribed total training duration, multiplied by 100.
Time Frame
During the intervention and T2: after finishing intervention (w 13)
Title
The presence of axillary web syndrome
Description
The diagnosis of Axillary Web Syndrome (AWS) will be made clinically. Scored on 5-point Likert scale (totally disagree, disagree, don't disagree/agree, agree, totally agree) The presence of rope-like cords in the axilla to the wrist is assessed by inspection and/or palpation.
Time Frame
T1: baseline (within one week before randomisation)
Title
The presence of lymphedema
Description
Lymphedema will be clinically diagnosed: The Stemmer sign is positive if the assessor is unable to pinch (between his/her thumb and index finger) the dorsal skin of proximal phalanx (second or third finger). A positive test confirms the presence of primary and secondary lymphedema of the arm(s). Single circumference measurement will only be performed if unilateral lymphedema is suspected. The arm circumference will be measured by a nylon tape measure with an accuracy of 1mm. The tape measure will be placed around the arm without tightening the tape at 30cm above the styloid process. Lymphedema is present if there is at least a difference of 10% between both arms.
Time Frame
T1: baseline (within one week before randomisation)
Title
The presence of arthralgia
Description
To assess arthralgia the assessor will ask the patient two questions: "Do you experience symmetrical pain in the left and right shoulders, elbows, wrists, fingers, hips, knees, ankles and/or toes?" and "Do you experience morning stiffness? And if so, for how many minutes?"
Time Frame
T1: baseline (within one week before randomisation)
Title
Detection of inflammation or adhesion of the scar tissue
Description
The scar tissue will be clinically scored. First, the assessor will inspect the affected (and painful) region for possible skin damage and will be looking for: wound disruption, hematoma (bruising), abscess (cavity filled with pus) and seroma (cavity filled with transparent liquid). Second, the he will inspect the presence of a possible inflammation process of the scar tissue and will be looking for signs such as: warmth, redness, etc. Third, he will assess the mobility of the scar. During this manual test, will be assessed whether the scar is moving relative to the underlying layers, which will be scored on a 5-point Likert scale with response possibilities: (totally disagree, disagree, don't disagree/agree, agree, totally agree).
Time Frame
T1: baseline (within one week before randomisation)
Title
Self-reported health care cost
Description
Measured with the 'Medical Consumption Questionnaire' 38 questions to quantify the direct medical costs of a patients' total medical consumption, encompassing additional diagnostics, consultations, surgery including stay in hospitals, physiotherapy, medication and aids prescribed by the general practitioner as well as medication and aids purchased by the patients themselves.
Time Frame
T1: baseline (within one week before randomisation), T2: after finishing intervention (w 13), T3: 3 months after intervention (w 26), T4: 1 year after intervention (w 64) and T5: 2 years after intervention (w 116)
Title
Self-reported work absenteeism and productivity loss at work
Description
Measured with the 'Productivity Cost Questionnaire' 20 questions to quantify the indirect costs outside health care but related to the disease (e.g. the costs due to absence of work and possible decreased productivity losses of paid and unpaid work).
Time Frame
T1: baseline (within one week before randomisation), T2: after finishing intervention (w 13), T3: 3 months after intervention (w 26), T4: 1 year after intervention (w 64) and T5: 2 years after intervention (w 116)
Title
Self-reported overall health status
Description
Measured with the 'EuroQol 5D instrument (EQ-5D-5L)' 5 dimensions scored on a 5-Likert scale and visual analogue scale (0 to 100) Higher score means a better outcome
Time Frame
T1: baseline (within one week before randomisation), T2: after finishing intervention (w 13), T3: 3 months after intervention (w 26), T4: 1 year after intervention (w 64) and T5: 2 years after intervention (w 116)
Title
Patient specific questionnaire
Description
Self-administered questions about: gender, ethnicity, age, nationality, weight, height, civil state, mutuality, educational level, year of the breast cancer diagnosis, received breast cancer treatments, lymphedema, medication, other treatments, menopausal, hot flashes.
Time Frame
T1: baseline (within one week before randomisation)

10. Eligibility

Sex
Female
Minimum Age & Unit of Time
18 Years
Accepts Healthy Volunteers
No
Eligibility Criteria
Inclusion Criteria: To meet the definition introduced by the National Cancer Institute's Office of Cancer Survivorship, in which a cancer survivor is a patient with a history of cancer that is beyond the acute diagnosis and treatment phase. Patients need to be cancer-free and should have finished their primary treatment with a curative intent for at least 3 months prior to study participation. Adjuvant hormonal therapy and immunotherapy form the exception to the rule and are tolerated. To report a pain severity of at least 3 out of 10 on pain visual analogue scale. To be able to speak and read in Dutch in order to give informed consent and to complete the assessment tools. Written and signed consent will be obtained from all participants. Exclusion Criteria: Suffering from dementia or cognitive impairment (unable to understand the test instructions and/or Mini Mental State Examination score <23/30). Suffering from severe psychological or psychiatric diseases. Diagnosis of new neoplasms or metastases.
Central Contact Person:
First Name & Middle Initial & Last Name or Official Title & Degree
Laurence Leysen, Dr.
Phone
+32 2477 43 26
Ext
Belgium
Email
Laurence.Leysen@vub.be
First Name & Middle Initial & Last Name or Official Title & Degree
Astrid Lahousse, Dra.
Phone
+32 2477 45 30
Ext
Belgium
Email
astrid.lucie.lahousse@vub.be
Facility Information:
Facility Name
Vrije Universiteit Brussel (VUB)
City
Jette
State/Province
Brussel
ZIP/Postal Code
1090
Country
Belgium
Individual Site Status
Recruiting
Facility Contact:
First Name & Middle Initial & Last Name & Degree
Laurence Leysen, PhD
Phone
+32 2477 43 26
Ext
Belgium
Email
laurence.leysen@vub.be
First Name & Middle Initial & Last Name & Degree
Astrid Lahousse, MSc
First Name & Middle Initial & Last Name & Degree
Jo Nijs, PhD
First Name & Middle Initial & Last Name & Degree
David Beckwée, PhD
First Name & Middle Initial & Last Name & Degree
César Fernández-de-las-Peñas, PhD
First Name & Middle Initial & Last Name & Degree
Laurence Leysen, PhD

12. IPD Sharing Statement

Learn more about this trial

The Effect of Pain Neuroscience Education and Behavioural Graded Activity on Chronic Pain in Breast Cancer Survivors

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