This prospective 2-phase study will use input from relevant stakeholders to refine the SMART-U intervention to ensure acceptability (Phase 1) and then test the effects of the intervention, reducing seizure frequency and improving other health outcomes (Phase 2).
Study objectives
-
To assess the efficacy of SMART- U vs. eTAU in a prospective randomised controlled trial.
We hypothesised that individuals randomised to SMART-U will have significantly improved QOL with fewer seizures, have greater improvement in depression and functional status compared to eTAU.
-
To use short message service (SMS) delivered via mobile phone text to validate patient self-reported seizure occurrence and push epilepsy self-management messaging in a practical/accessible format.
-
To obtain input from stakeholders (patients, family and clinicians) guided by an Integrated Promotion Action on Research Implementation in Health Services (i-PARIHS) framework to help establish sustainable infrastructure that will facilitate future scale-up of SMART in Uganda with epilepsy partners
Study setting
The study population will be drawn from neurology clinics where patients with epilepsy and epilepsy-related complications receive free treatment and supportive care at Mulago and Mbarara hospitals. Mulago and Mbarara hospitals are the only hospitals currently that run regular epilepsy clinics that are supported by neurologists in Uganda and tend to provide care for severe forms that are intractable. This offers an opportunity to study this intervention.
At Mulago, patients attending the neurology clinic are referred from medical wards, while others are referred from surrounding health centers for specialised care and treatment for epilepsy. The neurology clinic runs on Wednesdays from 9 am -2 pm with an average attendance of about 5–8 patients with confirmed epilepsy. These patients are then given scheduled visits unless certain illnesses warrant an unscheduled visit. Severely ill patients were referred to the respective wards for admission and in-patient care. A total of about 20–30 patients with epilepsy are seen in the neurology clinic monthly.
Mbarara Regional Referral Hospital is a public regional referral hospital for the districts of Mbarara, Bushenyi, Ntungamo, Kiruhura, Ibanda, and Isingiro, with an official bed capacity of 600. It is located in Mbarara a teaching hospital for the Mbarara University of Science and Technology. MRRH has neurology and psychiatry clinics staffed by physicians and nurses caring for PWE. A neurologist and medical officer run the clinic, equipped with an electroencephalogram with technicians and nurses for diagnosis and care. The clinic receives about 5–10 PWE weekly and 30 PWE monthly.
Study design
This prospective non-inferiority randomised clinical trial will be conducted at Mulago and Mbarara hospitals. Participants will be adults who meet the inclusion criteria from the epilepsy clinics at Mulago and Mbarara who will be approached to participate in the study and enrolled.
The estimated sample size for the study is 188 people with epilepsy, allowing for 20% attrition or loss by missing data, reducing the final sample to a minimum of N = 150 participants.
Based on a power analysis using G*Power 3.1.9.2121 for a 2 group by 3 time points (baseline, 13-week and 24-week follow-up) repeated measures analysis of variance (RMANOVA) with an alpha of 0.05, a power of. 80, for a sample of 150 we will be able to detect a small standardised effect size of 0.10 for the within-time effect, within the time-by-group interaction effect and a small to moderate standardised effect of 0.19 for the between-group effect.
Study population
All adult PWE attending the neurology clinics at Mulago and Mbarara hospitals during the study period who or their caregivers will be approached. All participants and their legal guardians will provide written informed consent. All consecutive patients who came either for follow-up or as new referrals with a confirmed diagnosis of epilepsy will be screened for inclusion in the study. We will include those who meet the following inclusion criteria: 1. Participants will have a clinical diagnosis of epilepsy documented with at least two outpatient visits; 2. aged more than 18 years; 3. provide written informed consent by the study participant or immediate caregiver/legal guardian; 4. Ability to participate in study procedures, 5. having had at least 1 seizure in the past 6 months; 6. Owning a mobile phone either by the PWE or immediate caregiver.
We will exclude those 1. Diagnosed with dementia, 2. Participants who are pregnant (given the likely need for different and more intensive treatments among pregnant PWE, may affect their ability to participate in the SMART-U sessions regularly and those unable to participate in study procedures.
Study procedures
Randomisation:
Participants will be randomly assigned in a ratio of 1:1 basis to receive either SMART-U (N = 94) or eTAU (N = 94) using block randomisation. Block randomisation with a random block size of 4 to 8 consecutive patients will be performed to ensure that equal numbers of SMART and ETAU patients occur within strata and are balanced. The randomisation list will be computer-generated by staff from the CWRU Neurological and Behavioural Outcomes Centre Biostatistical Core who are not part of the study staff.
SMART-U Intervention group:
The SMART-U self-management approach of the intervention uses nurses and peer educator dyads (PEDs) made up of patients and their care partners to deliver the intervention together. SMART-U begins with a 30-60-minute orientation session where the nurse and PED meet with the patient and their care partner. This is followed by 6 weekly, one-hour group sessions with 6–8 patients and their care partners. Topics covered are noted in Table 1 and are typically delivered over a period of 10–12 weeks. All SMART-U participants continue to receive treatment with their regular medical care providers.
Table 1
Topics addressed during SMART-U sessions.
Sessions | Activities/Topic |
Session 1 | Orientation and introductions; Emphasise ground rules; Establishment of a therapeutic relationship; Facts and myths about epilepsy, and general epilepsy management principles |
Session 2 | Relationship of epilepsy and stress; Stigma and “double stigma”; Strategies to cope with stigma; Introduction to personal goal setting |
Session 3 | Treatments for epilepsy; Complications of epilepsy; Minimising epilepsy complications; The importance of daily routine and good sleep habits |
Session 4 | Problem–solving skills and the IDEA approach (Identify the problem, define possible solutions, Evaluate the solutions, Act on the best solution); Talk with your healthcare providers; Role play of communication with care providers. |
Session 5 | Nutrition for the best physical and emotional health; Substance abuse and its effects on epilepsy; Specific stress–management approaches |
Session 6 | Effects of exercise and being outdoors on physical and emotional health; Medication routines; Prioritising medication side effects and discussing it with your clinician |
Session 7 | Social support and using your available supports; Advocacy groups for epilepsy; A personal care plan to take care of the mind and the body |
Session 8 | Normalising your life in spite of having a chronic but unpredictable condition; Self-management as a lifestyle; Acknowledgment of group process; Setting the stage for ongoing illness management and recovery. |
Control arm-Enhanced Treatment as Usual (eTAU) group:
Individuals randomised to eTAU will continue in their usual care supplemented by written materials on epilepsy in their preferred language and tailored to the reading level of most patients at the clinic. To control for the same number of patient contacts as SMART-U, the nurse in eTAU will follow up with participants with a series of 8 brief phone calls spaced out over the course of 6 months (approximately every 2 weeks during months 1 and 2, then approximately monthly thereafter).
SMS seizure monitoring and support:
During the 24-week duration of the trial, both SMART-U and eTAU participants will receive/use SMS to monitor/report seizure occurrence and duration. Participants will receive an automated weekly survey via SMS asking if they had a seizure in the past week.
Feasibility and Fidelity:
Acceptance will be assessed at the end of each series of 8 group sessions with a short self-assessment survey. Following Fraser, fidelity to the SMART-U intervention will be assessed quantitatively and qualitatively. Research staff not involved in the intervention will monitor and score at least 25% of the group sessions, rating each dimension of fidelity on a scale of 1 to 10. The feasibility of texting for both the SMART-U -U and eTAU groups will be assessed by the number of text responses/number of texts sent.
Qualitative evaluation:
We will use In-depth interviews on perceived benefits vs. burdens and barriers/facilitators to SMART-U, and eTAU implementation will be conducted at each of the 2 sites. Given the corrosive and persistent nature of stigma on QOL among PWE, input and recommendations on specific strategies regarding ways to potentially mitigate stigma in families and communities will be assessed. Informants will include 20 PWE from SMART-U and 20 PWE from eTAU (total N = 40). We will conduct qualitative interviews to elicit participant perceptions of the intervention at 13-weeks (when SMART-U groups are completed) and again at 24 weeks. For qualitative interviews, this sample size is within the range of recommended sample sizes (i.e., 20–50 individuals).
Study outcomes:
The Primary outcome will be Mean change in cumulative past 24-week seizure frequency (24 weeks prior to study baseline compared to the 24-week follow-up) and Mean change from baseline to 24 weeks in QOL. Additional secondary outcomes will include Mental health comorbidity, stigma, epilepsy self-management competency, and other relevant variables, which will be assessed using validated, standardised questionnaires.
Study Data:
Study questionnaires will be used for data collection. Study teams will be based within the neurology outpatient clinics; an interviewer will administer the questionnaire and will record answers on the paper questionnaire. Data captured will be entered into a Microsoft Access database by the entry clerk and double-entered to ensure accuracy. Back-up database files will be kept at the end of each data entry session. For quality control purposes, query programs will be written into the database to limit the entry of incorrect data and ensure data entry into the required fields.
Data Storage:
Source data in this study will include survey questionnaires and investigation results. All study documents will be kept in secure filing cabinets in the offices at Makerere University, College of Health Sciences. The principal investigator will be responsible for the security of all study documents.
Quality Control:
All study team members will be trained in the project objectives, methods of effective communication with study participants and collection of high-quality data. The study team will receive additional training specific to the tasks they will perform within the project, including interview techniques, administration of surveys, and completion of questionnaires. Standard Operating procedures (SOPs) will be written for project activities, and booklets of all relevant documents will be provided to each member of the project team.
Data analysis and Data management:
The investigators at each study site will oversee data input and quality and, working with the study statistician and epidemiologist, will oversee the quantitative data analytic procedures. The CWRU data management and statistics team will also provide data management consultation as appropriate. Rigorous development of data collection forms and staff training on properly completing and checking data collection forms will reduce errors at the point of collection. Additional data management practices before and after entry into the RedCap database will identify potential problems or outlying values and catch other errors on data collection forms. Data management staff will be responsible for tracking forms entered and performing routine data checks. Analytic data sets will be prepared using SAS 9.4
Repeated Measure Analysis of Variance. The primary outcomes of interest are quality of life (QOL) and cumulative seizure frequency. Three different analytic strategies will be used to assess AIM 1. Cumulative seizure frequency will be assessed with independent samples t-tests and linear regressions, while QOL and the secondary outcomes will be examined using repeated measures analysis of variance (RMANOVA). We will examine 2 different sets of RMANOVAs.
Qualitative data analysis plan
Qualitative data analysis. Interview theme analysis will be conducted with accepted qualitative data analysis methods, including specialised software, calculation of inter-rater reliabilities, rater calibration, and systematic synthesis of findings. Additional methodologic detail is provided in the data analysis section.
Adverse event identification/classification:
The study investigators and/or qualified research assistants will identify adverse events. All adverse events, whether considered serious or not, will be recorded and reviewed by the study P.I.s on an ongoing basis and reported to the IRB according to local IRB policy. Serious adverse events (A.E.s) are defined as events that result in any of the following: death; a life-threatening experience; in-patient hospitalisation or prolongation of existing hospitalisation; a persistent or significant disability/incapacity; or a congenital anomaly/birth defect (or an event that may require medical or surgical intervention to prevent one of the outcomes listed above).
Seizures, as a defining hallmark of epilepsy, will be recorded if/when they occur but will not be considered either SAEs or A.E.s. All A.E.s, including all SAEs, will be reported to the IRB according to local IRB policy and to the Data Safety and Monitoring Board (DSMB). A summary report of all adverse events will be submitted annually in the report and at the end of the study.
Data and safety monitoring Board (DSMB) and safety review plan
The study will have a DSMB composed of members who are not part of the study team. At a minimum, they will review and evaluate the accumulated data for participant safety, A.E.s, study conduct and progress every 12 months. Ad-hoc meetings might be called to evaluate unanticipated serious adverse events or any other urgent issues that are relevant and which might occur during the course of the study. The DSMB will be comprised of two clinicians with epilepsy expertise at the Uganda site, a faculty member/clinician with epilepsy expertise at the U.S. site, and a biostatistician at the U.S. site who are all not part of the study team but have extensive experience with federally funded research. The DSMB communication and oversight will be accomplished via videoconference or email communication for issues needing immediate attention.
Ethics and Dissemination
The study will be conducted according to the Helsinki Declaration[12], the NIH Human Subjects guidelines, and the International Conference on Harmonization E6 Guideline for Good Clinical Practice [13]. Approvals from local leaders will be sought before the study activities commence in the proposed areas. The study nurses will obtain informed consent from potential participants before study procedures are initiated. A copy of the consent form will be given to the study participant. Patient identifiers at the analytic level will differ from the patient’s clinic medical record number. The files that link the patient identifiers to the study numbers will be kept in locked cabinets in the study staff offices. Only aggregate data will be presented, published, and presented such that individual patients cannot be identified. This protocol version 2 dated 29th Sept 2023 was approved by the School of Medicine, Research and Ethics Committee (SOMREC) Mak-SOMREC-2023-648 and UNCST; HS2944ES. The results of this study will be submitted for publication in peer-reviewed journals, and the key findings will be presented at national conferences.