ANZCTR - Registration

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Trial registered on ANZCTR

Registration number

ACTRN12620000550909

Ethics application status

Approved

Date submitted

3/04/2020

Date registered

11/05/2020

Date last updated

10/10/2022

Date data sharing statement initially provided

11/05/2020

Type of registration

Prospectively registered

Titles & IDs

Public title

Assessing a new treatment for Functional Neurological Symptoms Disorder (FNSD): a randomised controlled trial.

Scientific title

Effect of Nocebo-Hypothesis Cognitive Behavioural Therapy (NH-CBT) on physical functioning in patients with Functional Neurological Symptoms Disorder (Motor Type): a randomised controlled trial

Secondary ID [1]

Health Research Council of New Zealand Reference Number: 20/045

Universal Trial Number (UTN)

U1111-1249-5358

Trial acronym

NHCBT

Linked study record

Health condition

Health condition(s) or problem(s) studied:

Functional Neurological Symptoms Disorder

Condition category

Condition code

Neurological

Other neurological disorders

Physical Medicine / Rehabilitation

Other physical medicine / rehabilitation

Intervention/exposure

Study type

Interventional

Description of intervention(s) / exposure

The current intervention is based on the idea that functional neurological symptoms occur as the result of a nocebo effect. In other words, a subconscious belief/representation of being neurologically damaged produces symptoms.
The intervention is administered on an individual basis. It includes an explanation of the “nocebo hypothesis” to the patients within the context of a personalised psychosocial formulation of their symptoms by a clinical psychologist. Physical therapy then follows, incorporating video recording and feedback to show the patient that their functioning can improve when they are distracted (e.g. by music). These therapy elements are designed in order to weaken people's belief that they are neurologically damaged, and give a clear alternative explanatory account of causation. The physical therapy elements of the treatment will be delivered by rehabilitation professional, including a physiotherapist.
Patients will receive written information about their diagnosis and treatment, consistent with the education given to them. Dependent on individual patient need (e.g. type and severity of symptoms), the following equipment may potentially be used: mobility aids (e.g. walking frame), parallel bars, treadmill, portable electromyography biofeedback unit.
The intervention will be delivered face to face over 8 weeks (minimum of 3 hours up to a maximum of 25 hours total duration, session duration 45 - 90 minutes). The frequency and scheduling will depend on the patient’s stamina and needs. Sessions will follow a standardized script/format and will be part of either an inpatient or outpatient treatment.
All therapists in this trial have to study a therapy manual and receive a training in the treatment content and procedure. Therapists are required to attend supervision frequently with a licensed supervisor experienced in CBT for patients with functional neurological symptoms. All initial therapy sessions will be video-taped, and the first physical therapy session will also be audio-taped. We will design a rating scale to assess treatment fidelity and its two components, therapist adherence and treatment specificity, for both the NH-CBT and the control intervention. We will assess therapist competence with a validated rating scale. Session records of a randomly selected sample (30% of the intention-to-treat [ITT] sample) will be rated by an independent, blinded rater.
The majority of sessions will occur at the ISIS (Rehabilitation) Centre, Wakari Hospital, Dunedin, for both inpatient and outpatient treatment, although some sessions will occur in community settings for some patients, predominantly when they are in the latter stages of treatment.

Intervention code [1]

Rehabilitation

Intervention code [2]

Treatment: Other

Comparator / control treatment

The active control treatment is based on (but not identical to) an established physical therapy intervention (for functional neurological symptoms) embedded in psychoeducation (see PHYSIO4FMD trial, Nielsen et al 2019). There will be some initial supportive counselling and basic information giving with a psychologist. Subsequent physical therapy will largely consist of ‘movement retraining’ (i.e. increasingly establishing symptom free components of movement), tailored to the individual, but adhering to the key principle of employing strategies that redirect the patient’s focus of motor attention, e.g. they might focus on the goal of the task rather than the mechanics of movement, or their reflection in a mirror. Neither highly engrossing distractors nor the use of video feedback will be permitted.
Materials / equipment used will be otherwise identical to the intervention condition, except there will be no use of a tablet for video feedback, or a portable EMG biofeedback unit.
Patients will receive written information about their diagnosis and treatment, consistent with the education given to them in the control condition.
Treating staff type (by training), location, duration of sessions and overall treatment duration will be identical to the intervention condition.

At 16 weeks post-commencement of control treatment, control participants will be offered the intervention condition if they have not achieved full symptom remission.

Control group

Active

Outcomes

Primary outcome [1]

Physical functioning, as measured by the Short Form 36 - Physical Functioning subscale (self-rated)

Timepoint [1]

Baseline, then 8 weeks (primary time point), 16 weeks and 24 weeks (control group only) post-commencement of intervention.

Secondary outcome [1]

Somatic symptom severity, as measured by a modified version of the Patient Health Questionnaire-15 (self-rated)

Timepoint [1]

Baseline, then 8 weeks, 16 weeks and 24 weeks (control group only) post-commencement of intervention.

Secondary outcome [2]

Patient perception of change, as measured by the Clinical Global Impression Scale of Improvement scale (CGI-I)(self-rated)

Timepoint [2]

8 weeks, 16 weeks and 24 weeks (control group only) post-commencement of intervention.

Secondary outcome [3]

Mobility, as measured by the 10 metre Walk Test (10MWT)(observer rated)

Timepoint [3]

Baseline, then 8 weeks, 16 weeks and 24 weeks (control group only) post-commencement of intervention.

Secondary outcome [4]

Mobility, as measured by the Functional Mobility Scale (observer rated)

Timepoint [4]

Baseline, then 8 weeks, 16 weeks and 24 weeks (control group only) post-commencement of intervention.

Secondary outcome [5]

Health care utilisation, as measured by hospital and GP data regarding presentations to services, as well as questions 7 and 8 from the Client Service Receipt Inventory (CSRI) (self-rated)

Timepoint [5]

Baseline, then 16 weeks post-commencement of intervention.

Secondary outcome [6]

Illness perception, as measured by the Brief Illness Perception Questionnaire (B-IPQ)(self-rated)

Timepoint [6]

Baseline, then 8 weeks, 16 weeks and 24 weeks (control group only) post-commencement of intervention.

Secondary outcome [7]

Health-related quality of life, as measured by the Short Form 36 (SF36)(self-rated).

Timepoint [7]

Baseline, then 8 weeks, 16 weeks and 24 weeks (control group only) post-commencement of intervention.

Secondary outcome [8]

Quality of life, measured using the EQ-5D-5L (self-rated).

Timepoint [8]

Baseline, then 8 weeks, 16 weeks and 24 weeks (control group only) post-commencement of intervention.

Secondary outcome [9]

Fatigue, as measured by the Vitality Scale of the Short Form 36 (SF36)(self-rated).

Timepoint [9]

Baseline, then 8 weeks, 16 weeks and 24 weeks (control group only) post-commencement of intervention.

Secondary outcome [10]

Catastrophic thinking about symptoms, as measured by the Symptom Catastrophising Scale (self-rated).

Timepoint [10]

Baseline, then 8 weeks, 16 weeks and 24 weeks (control group only) post-commencement of intervention.

Secondary outcome [11]

Anxiety, as measured by the Generalised Anxiety Disorder scale (GAD-7)(self-rated).

Timepoint [11]

Baseline, then 8 weeks, 16 weeks and 24 weeks (control group only) post-commencement of intervention.

Secondary outcome [12]

Depression, as measured by the Patient Health Questionnaire-9 (PHQ-9)(self-rated).

Timepoint [12]

Baseline, then 8 weeks, 16 weeks and 24 weeks (control group only) post-commencement of intervention.

Secondary outcome [13]

Dissociation, as measured by the Brief Dissociative Experiences Scale (DES-B)(self-rated).

Timepoint [13]

Baseline, then 8 weeks, 16 weeks and 24 weeks (control group only) post-commencement of intervention.

Secondary outcome [14]

Symptom disability, as measured by the Pain Disability Index (self-rated).

Timepoint [14]

Baseline, then 8 weeks, 16 weeks and 24 weeks (control group only) post-commencement of intervention.

Secondary outcome [15]

Therapeutic alliance, as measured by the Work Alliance Inventory - Short Form (WAI-SF)(self-rated).

Timepoint [15]

8 weeks post-commencement of intervention.

Secondary outcome [16]

Adverse events in therapy (particularly ruptures in the therapeutic alliance), as measured by the Inventory for the balanced assessment of Negative Effects of Psychotherapy (INEP)(self-rated).

Timepoint [16]

8 weeks and 24 weeks (control group only) post-commencement of intervention.

Secondary outcome [17]

Adverse events in therapy (particularly physical injury and near misses), as measured by Severity Assessment Code rating for adverse event reporting (observer rated)

Timepoint [17]

8 weeks and 24 weeks (control group only) post-commencement of intervention.

Secondary outcome [18]

Functional Neurological Symptoms, as measured by the Simplified Functional Movement Disorder Rating Scale (S-FMDRS)(observer rated)

Timepoint [18]

Baseline, then 8 weeks, 16 weeks and 24 weeks (control group only) post-commencement of intervention.

Eligibility

Key inclusion criteria

Patients that will be included in our trial will have to meet the following criteria:
• aged 18 or older
• have been assessed by a neurologist including the appropriate medical investigation (e.g. imaging), and that assessment will have resulted in a formal diagnosis of FNSD (i.e. they meet DSM-V diagnostic criteria), or will have clearly identified functional neurological symptoms (according to Fahn-Williams / Gupta-Lang criteria).
• have consented to participate

Minimum age

18 Years

Maximum age

No limit

Sex

Both males and females

Can healthy volunteers participate?

Key exclusion criteria

Patients will be excluded from the trial if they meet the following criteria:
• they have a diagnosis of complex regional pain syndrome (CRPS)
• they have a diagnosis of Dissociative Identity Disorder (DID)
• they have a diagnosis of Post-Traumatic Stress Disorder (PTSD) with high severity and significant dissociation.
• they require inpatient mental health treatment during the trial.
• they receive psychopharmacotherapy and change their treatment regimen from four weeks before baseline assessment until the final assessment.
• according to the clinical judgement of the lead investigator, there are concerns about their ability to participate fully in the trial, e.g. they have active and extensive self-harm, or frequent admissions for inpatient mental health treatment in the last two months
• they sustain significant physical trauma during the period of the trial (inside or outside of the treatment setting), and therefore cannot participate in the physical therapy.
• their English language proficiency is low.
• they do not have the capacity to consent to participating in the trial
• they have previously received either NH-CBT or the active control treatment

Study design

Purpose of the study

Treatment

Allocation to intervention

Randomised controlled trial

Procedure for enrolling a subject and allocating the treatment (allocation concealment procedures)

Eligible participants will undergo baseline assessment by an independent assessor, before being randomly assigned to one of the study arms. Allocation will be concealed in sealed opaque sequentially number envelopes.

Methods used to generate the sequence in which subjects will be randomised (sequence generation)

The randomisation will be conducted by a research associate not affiliated with the study. Randomization will be obtained by an online service which uses a pseudorandom number algorithm (e.g. www.randomization.com).

Masking / blinding

Blinded (masking used)

Who is / are masked / blinded?

The people receiving the treatment/s

The people assessing the outcomes

Intervention assignment

Parallel

Other design features

If participants in the control group have not achieved full symptom remission at 16 weeks post-commencement of intervention, they will receive NH-CBT for a maximum of 25 more hours. They will then be assessed again, using largely the same measures

Phase

Not Applicable

Type of endpoint/s

Safety/efficacy

Statistical methods / analysis

The power analysis for our trial was run with G*Power 3.1.9.4. In a previous trial, our control treatment reached moderate effect (f=0.33) at 6-month follow-up on the SF36 physical function subscale, our primary outcome (Nielsen et al, 2017) For this trial we conservatively assume a small group*time interaction effect (f=0.10) under consideration of our three measurements and a test-retest reliability of r=0.5. A power analysis for a mixed-effect ANOVA with an alpha error probability of 0.05 and a power of 0.80 results in an optimal total sample size of 164.

Statistical analyses will be run with IBM SPSS Statistics. All of our analyses will be based on intention-to-treat principle. Multiple imputation procedure offered by IBM SPSS Statistics will be used to replace missing values. Group*time interaction effects as well as main group and time effects for our primary and secondary outcomes will be analysed with mixed-effect univariate ANOVAs with one within group factor (baseline, post-treatment, 6-month follow-up) and one between-group factor (NH-CBT versus control intervention). Significant interaction effects will be broken down with Bonferroni-corrected post hoc pairwise comparisons of cell means.

Recruitment

Recruitment status

Recruiting

Date of first participant enrolment

Anticipated

25/05/2020

Actual

19/06/2020

Date of last participant enrolment

Anticipated

31/10/2022

Actual

Date of last data collection

Anticipated

20/02/2023

Actual

Sample size

Target

164

Accrual to date

Final

Recruitment outside Australia

Country [1]

New Zealand

State/province [1]

Otago

Funding & Sponsors

Funding source category [1]

University

Name [1]

University of Otago

Address [1]

Research and Enterprise Department,
Health Research South
Dunedin School of Medicine
1st floor, Dunedin Public Hospital
201 Great King Street
Dunedin 9016

Country [1]

New Zealand

Primary sponsor type

Individual

Name

Dr Matt Richardson

Address

Department of Psychological Medicine
Dunedin School of Medicine
University of Otago
PO Box 56
Dunedin 9054

Country

New Zealand

Secondary sponsor category [1]

Individual

Name [1]

Dr Maria Kleinstaeuber

Address [1]

Department of Psychological Medicine
Dunedin School of Medicine
University of Otago
PO Box 56
Dunedin 9054

Country [1]

New Zealand

Other collaborator category [1]

Individual

Name [1]

Dr Dana Wong

Address [1]

School of Psychology and Public Health
La Trobe University
Plenty Road and Kingsbury Drive
Bundoora
VICTORIA 3086

Country [1]

Australia

Other collaborator category [2]

Individual

Name [2]

Professor Paul Glue

Address [2]

Department of Psychological Medicine
Dunedin School of Medicine
University of Otago
PO Box 56
Dunedin 9054

Country [2]

New Zealand

Ethics approval

Ethics application status

Approved

Ethics committee name [1]

Health and Disability Ethics Committee

Ethics committee address [1]

Ministry of Health
Health and Disability Ethics Committees
PO Box 5013
Wellington 6140

Ethics committee country [1]

New Zealand

Date submitted for ethics approval [1]

02/04/2020

Approval date [1]

14/04/2020

Ethics approval number [1]

20/STH/56

Summary

Brief summary

The main purpose of the study is to see if the treatment improves physical functioning in people with functional neurological symptoms - in other words, reduces or eliminates their symptoms.

The treatment starts with a session with a psychologist, who listens to the patient's situation, and then explains why their symptoms might have started in the first place, and why they are still there. The patient then receives physical therapy sessions, e.g. focusing on getting their affected limbs moving again. Patients are distracted at certain times (e.g. with music) to see if that helps start to reduce symptoms. They are encouraged to attempt more and more difficult physical tasks as they start to recover.

Trial website

Trial related presentations / publications

Public notes

It should be acknowledged that the COVID-19 outbreak may significantly impact this study in terms of reducing the recruitment period. As a contingency plan, if the required number of participants are not recruited to enable the above type of analysis, then analysis will instead focus on effect size calculations rather than significance testing. These effect sizes can be used for a power analysis for a larger definitive trial in future

Contacts

Principal investigator

Name

Dr Matt Richardson

Address

Department of Psychological Medicine
Dunedin School of Medicine
University of Otago
PO Box 56
Dunedin 9054

Country

New Zealand

Phone

+64 27 458 5634

Fax

[email protected]

Contact person for public queries

Name

Dr Matt Richardson

Address

Department of Psychological Medicine
Dunedin School of Medicine
University of Otago
PO Box 56
Dunedin 9054

Country

New Zealand

Phone

+64 27 458 5634

Fax

[email protected]

Contact person for scientific queries

Name

Dr Matt Richardson

Address

Department of Psychological Medicine
Dunedin School of Medicine
University of Otago
PO Box 56
Dunedin 9054

Country

New Zealand

Phone

+64 27 458 5634

Fax

[email protected]

Data sharing statement

Will individual participant data (IPD) for this trial be available (including data dictionaries)?

Yes

What data in particular will be shared?

Individual participant data that underlie the results reported in this article, after de-identification (text, tables, figures, and appendices).

When will data be available (start and end dates)?

Immediately following publication; no end date.

Available to whom?

Researchers who provide a methodologically sound proposal for re-analyses.

Available for what types of analyses?

For re-analyses, if their aim is covered by the purpose described and agreed on in the patient information sheet and informed consent.

How or where can data be obtained?

Proposals should be directed to the Principal Investigator ([email protected]). To gain access, data requestors will need to sign a data access agreement. Data are not publicly available because informed consent provided by participants of this study is committed to a defined purpose.

What supporting documents are/will be available?

Doc. No.	Type	Citation	Link	Email	Other Details	Attachment
7489	Study protocol			[email protected]

Results publications and other study-related documents

Documents added manually

No documents have been uploaded by study researchers.

Documents added automatically

Source	Title	Year of Publication	DOI
Embase	Nocebo-Hypothesis Cognitive Behavioral Therapy (NH-CBT) for Persons With Functional Neurological Symptoms (Motor Type): Design and Implementation of a Randomized Active-Controlled Trial.	2020	https://dx.doi.org/10.3389/fneur.2020.586359

N.B. These documents automatically identified may not have been verified by the study sponsor.

Trial Review

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Documents added automatically