Adapted Solution Focused Therapy for People With Aphasia (SOFIA Trial)

Not Applicable

Completed

• Conditions: Stroke; Aphasia
• Interventions: Behavioral: Adapted Solution Focused Brief Therapy

• Registration Number: NCT03245060
• Lead Sponsor: City, University of London

Brief Summary

Around one third of stroke survivors will have aphasia, which means they will have difficulty talking, understanding, reading or writing. The main aims of this study are to assess: \[1\] the acceptability of an existing psychosocial intervention, solution focused brief therapy, to people with varying presentations of aphasia; and \[2\] the feasibility of conducting a future definitive trial investigating clinical and cost effectiveness.

Detailed Description

Background and Aims Around one third of people who have a stroke will experience aphasia, a language disability that can affect talking, understanding, reading or writing. The psychosocial impact of aphasia is considerable: those living with chronic aphasia are at risk of social isolation and depression. One potential intervention is Solution Focused Brief Therapy (SFBT). SFBT is an approach to building positive change in a person's life. It builds up a picture of a client's preferred future; encourages a person to notice positive signs of change; explores personal resources, skills and resilience; and acknowledges the impact of the stroke on a person's life and identity.

The current project builds on a small-scale proof-of-concept study that explored SFBT with five people who had mild to moderate aphasia, at least two years post stroke. There were improvements in participants' mood and participation and participants found the therapy highly acceptable.

The main aims of the current project are to assess: \[1\] the acceptability of SFBT to people with varying presentations of aphasia; and \[2\] the feasibility of conducting a future definitive trial investigating clinical and cost effectiveness.

Methods The overall study will last for 38 months (November 2016 to December 2019), and comprise a Development Phase (year 1) and a single-blind, randomized, wait-list controlled, feasibility trial with nested qualitative research comparing SFBT plus usual care to usual care alone (years 2 and 3).

During the Development Phase the investigators will develop the therapy manual and fidelity checking processes, train the clinicians, and finalize the protocol. Phase One has been informed through four workshops with the Aphasia Advisory Group, comprised of four people with aphasia and one carer, who advised on the study protocol and trial documentation. The investigators also conducted a pilot study with four people who have severe expressive and receptive aphasia where the investigators trialed the assessment and therapy protocol, and explored adapting the therapy for people with severe communication difficulties.

For the feasibility trial (commencing October 2017) 32 participants will be recruited with any severity of aphasia, at least six months post stroke. Participants will be randomly assigned to the intervention group or wait-list control group. Both groups will be assessed by a Research Assistant blinded to treatment allocation on psychosocial outcome measures at T1 (baseline, prior to randomization), T2 (three months post randomization) and T3 (six months post randomization). Participants will also take part in in-depth interviews at T3 exploring their experiences of taking part in the project as well as complete a resource use questionnaire. All participants will receive all usual care, and up to six SFBT sessions spaced over three months delivered by Speech and Language Therapists. The intervention group will receive the therapy immediately post randomization, while the wait-list control group will be offered the intervention after T3. The wait-list control will additionally be reassessed at T4 (nine months post randomization). The investigators will also interview the trial clinicians, and the Local Collaborators at the two participant identification sites.

Results The feasibility of recruitment and retention of participants (including proportion who consent; rate of consent; attrition rates) will be assessed, as will treatment fidelity. Descriptive statistics for the clinical outcome measures will be presented, for the entire trial population and by trial arm, at each time point, with means and confidence intervals plotted over time. The proportion of missing data will also be reported. As part of the economic evaluation, the relevant costs and health gains will be presented by trial arm and the completeness of data collection methods and their acceptability will be assessed. Qualitative data on acceptability of the intervention and study procedures will be analysed using Framework Analysis.

Clinical Implications This trial has been designed to assess the acceptability of the intervention for people with varying presentations of aphasia, and the feasibility of conducting a successful definitive trial evaluating clinical and cost effectiveness in the future. Given the high levels of distress and isolation experienced by people living with aphasia, and the current poor evidence base, there is a pressing need to investigate effective psychosocial interventions. SFBT is potentially a relatively brief approach deliverable by Speech and Language Therapists.

Study Timeline

• Study First Submitted: 2017-08-04
• Study First Submitted QC: 2017-08-09
• Study First Posted: 2017-08-10
• Study Start: 2017-10-17
• Status Verified: 2019-01
• Primary Completion: 2019-08-14
• Study Completion: 2019-08-14
• Last Update Submitted: 2020-02-07
• Last Update Posted: 2020-02-10

Recruitment & Eligibility

• Status: COMPLETED
• Sex: All
• Target Recruitment: 32

Inclusion Criteria

Not provided

Exclusion Criteria

• Other diagnoses affecting cognition such as dementia or advanced Parkinson's Disease
• Severe uncorrected visual or hearing problems that would impact on a person's capacity to take part in the intervention
• Severe or potentially terminal co-morbidity on grounds of frailty
• Currently receiving a psychological or psychiatric intervention
• Non-fluent English speaker prior to the stroke based on self/family report
• Do not have mental capacity to consent to take part in the trial

Study & Design

• Study Type: INTERVENTIONAL
• Study Design: PARALLEL

Arm && Interventions

Group	Intervention	Description
Intervention: delayed SFBT	Adapted Solution Focused Brief Therapy	The wait-list control arm will receive the same intervention (Adapted Solution Focused Brief Therapy, SFBT) as the intervention arm, but after a delay of six months. Participants will also receive all usual care.
Intervention: immediate SFBT	Adapted Solution Focused Brief Therapy	The Intervention arm will receive up to six Adapted Solution Focused Brief Therapy (SFBT) sessions immediately post randomisation. The sessions will be spaced over 3 months. Participants will also receive all usual care.

Primary Outcome Measures

Name	Time	Method
Warwick Edinburgh Mental Well-being Scale (WEMWBS)	6 months post randomization	Measures mental well-being. 14 items, scores range from 14 to 70, with higher scores indicating greater overall mental well-being

Secondary Outcome Measures

Name	Time	Method
Warwick Edinburgh Mental Well-being Scale (WEMWBS) - measuring change	All participants will complete WEMWBS at baseline, pre-randomization (T1), 3 months post randomization (T2), 6 months post randomization (T3). The wait-list control arm will also be tested at 9 months post randomization (T4).	Measures mental well-being. 14 items, scores range from 14 to 70, with higher scores indicating greater overall mental well-being
Communicative Participation Item Bank (CPIB) - measuring change	All participants will complete CPIB at baseline, pre-randomisation (T1), 3 months post randomisation (T2), 6 months post randomisation (T3). The wait-list control arm will also be tested at 9 months post randomisation (T4).	Measures communicative participation. 10 items, scores range from 0 to 30 with higher scores indicating communication difficulties interfere less with participation
General Health Questionnaire-12 (GHQ-12) - measuring change	All participants will complete GHQ-12 at baseline, pre-randomisation (T1), 3 months post randomisation (T2), 6 months post randomisation (T3). The wait-list control arm will also be tested at 9 months post randomisation (T4).	Measures psychological distress. 12 items, scores range from 0 to 12 with higher scores indicating greater levels of distress
Depression Intensity Scale Circles (DISCS) - measuring change	All participants will complete DISCS at baseline, pre-randomisation (T1), 3 months post randomisation (T2), 6 months post randomisation (T3). The wait-list control arm will also be tested at 9 months post randomisation (T4).	Measures depression. Single item scale, scores range from 0 to 5, with a score 0-1 indicating no/low distress, and 5 high distress; designed to be accessible to people with cognitive or communicative deficits.

Trial Locations

Locations (1)

City, University of London; 🇬🇧 London, United Kingdom