Study setting & design
The study is a cluster-randomised trial with primary endpoint at 3 months’ post-randomisation. It will be conducted among 1200 PLWH attending 40 clusters (PHCFs) that provide HIV care. To be eligible, randomly selected PHCFs have to offer HIV care and treatment services to at least 100 PLWH. Eligible clinics will be selected from the 51 PHCFs in the three study districts of Wakiso and Masaka (semi-urban and rural) and Kalungu (rural) which in addition to treating other medical conditions provide HIV care to between 50 to 13,000 PLWH per PHCF depending on size. Randomisation will be completed by an independent statistician using a list of random numbers generated by statistical software (Stata 16.1 SE), and will be stratified by type of health facility (health centres versus hospitals). Within each stratum, clinics will be randomised in a 1:1 ratio to either the Collaborative Stepped Care arm (CSC arm; to receive EUC plus the HIV+D intervention) or the EUC arm (Figure 1). A minimum of 10 and a maximum of 30 eligible DD positive study participants will be enrolled per participating PHCF. The reporting of the trial will be in accordance with the SPIRIT guidelines for interventional trials (40) (Appendix 1).
Participant eligibility criteria and recruitment
Inclusion criteria
PLWH who have been on ART for at least 6 months, ≥18 years, residing in the study area, medically stable (not too ill to require emergency admission) at the time of the study, conversant in English or Luganda (the predominantly used local language), willing to be home visited (in instances of loss to follow up) and able to give informed consent will be eligible for enrollment if they score >10 on the PHQ-9.
Exclusion criteria
Potential participants who meet the above inclusion criteria but have impairments that hinder engagement with the research procedures for any reason (e.g. is deaf or hard of hearing, speech impaired, blind or partially sighted), unable to give informed consent, are already receiving treatment for depression or any psychiatric treatment before the trial and those with alcohol use problem will be excluded.
Recruitment
A health talk about depression will be given by the LHW to PLWH sitting in the triage area of the participating PHCFs. Thereafter, consecutive attenders will be approached and requested to be screened for the study until the day’s target is reached (4-5 PLWH who have a PHQ-9 score of ≥ 10), screening will be undertaken by the LHW. Selected study respondents will be screened for depression using the PHQ-2, a two-item questionnaire that assess for ‘depressed mood’ and ‘loss of interest in typically pleasurable activities’. Those who screen positive (PHQ-2 score >3) will be invited for further evaluation by the LHW for trial eligibility and consent. Eligibility assessment will include confirmation of DD using the PHQ-9 (41).
Interventions
All participants in the trial will receive Enhanced Usual Care. Usual mental health care in the HIV care situation of Uganda and many other sub-Saharan African settings, is effectively no mental health care. This is primarily because DD is not routinely assessed for or diagnosed. In this study, enhanced usual care will be provided - defined by i) providing the DD screening results to the attending clinician and ii) providing mhGAP training to attending clinicians for the target disorders including guidelines on when and where to refer patients for psychiatric care.
In addition to EUC, providers in the intervention arm clinics will receive training in mhGAP and the HIV+D intervention. The HIV+D intervention will consist of evidence-based treatments for depression (psychoeducation, behavioural activation and antidepressant medications) delivered in a stepped care format and overseen by an HIV counsellor/case manager. The HIV+D intervention will be delivered in 4 steps. Step 1 (initiation of treatment), patients with PHQ-9 scores of 10-19 are told of their scores and offered psychoeducation by a LHW. Step 2 (management of moderate to severe cases), patients who remain symptomatic at follow up (PHQ-9 score ≥5 after 4 weeks) will be offered BA; 4-10 sessions) by a LHW. Step 3 (monitoring outcomes), if after 6 sessions of BA, PHQ-9 scores are >10, the advice is to continue BA sessions to completion and add antidepressant medication (Fluoxetine 20mg/day for 6 months), initiated by the HIV clinician. Step 4 (referral to mental health worker), if there is no improvement (PHQ-9>5) after step 3 or at eligibility assessment PHQ-9>20, or if someone has a high suicide risk (based on suicide risk assessment using the suicidality module of the Mini International Neuropsychiatric Interview (MINI) (42) by the supervisor for those who score ≥ 1 on item 9 of the PHQ-9 which reads, ‘over the last 2 weeks, how often have you had thoughts that you would be better off dead or of hurting yourself in some way?), continue all existing treatment and refer to a mental health worker.
To recruit LHW for this study, a local advert will be run at each of the participating PHCF. Minimum qualifications will include at least 11 years of formal education and a certificate of good conduct from the Local Council I (LC I) leadership, previous training and work in a counsellor role will be an added advantage. Training of LHW will employ both didactic methods and the use of role plays. Supervision of LHWs will be undertaken by the supervising HIV counsellor including through weekly supervision meetings where samples of audio-recordings of the therapy sessions will be listened to and feedback provided.
Fidelity to the intervention
To ensure fidelity in the delivery of the treatment by LHW, the BA therapy sessions have been manualised and all therapy sessions with clients will be audio-recorded. A random sample of these recordings will be discussed with the case manager at weekly clinic meetings. Quantity and quality level fidelity indicators of the treatment will be collected and evaluated. Quantity indicators will be obtained from the study participants’ case records where the types of treatment offered, number of sessions per treatment provided and duration of treatment sessions, will be routinely collected by standardised questionnaire. Quality indicators will be assessed through ratings of 10% of the audio-recording of all sessions by independent assessors blind to outcome data using standardised quality assessment questionnaires.
Treatment monitoring and discharge from treatment
The recruited study participants will be followed for 12 months’ post-randomisation. The monitoring schedule in the intervention arm will include assessment at 4, 16 and 40 weeks respectively. At these assessment points, the intervention team (LHW and their supervisors) will decide whether the patient should be considered for discharge (PHQ-9<5) or stepped up to the next level of care. Patients will be discharged from treatment if their PHQ-9 scores remain below 5 at a follow-up review 4 weeks after a scheduled monitoring visit. Participants with a high suicide risk at any assessment point will be referred to the mental health worker.
Study outcomes measures
The study outcome measures will be collected by means of questionnaires that will be administered to study participants by trained research assistants (TRA) who will be separate from the study implementation team. Data collection by TRA will be supported and overseen by Research Supervisors (RS; trained psychiatric nurses or psychiatric clinical officers who will each oversee four study PHCFs). The three-month outcome is the primary end-point of the trial as majority of study participants will have completed their BA sessions and we would expect the optimal effect of the treatment. The 12-month end-point is included to evaluate the sustainability of the effect of the intervention. The outcome assessment measures with the specific outcomes are summarised in Table 1. The primary outcome measure in this study will be the mean DD symptom severity scores (assessed using the PHQ-9) at 3 months.
Table 1: HIV+D outcome measures and specific outcomes
Outcome
|
Source of data
|
Endpoint
|
Collected at 3 months
|
Collected at 12 months
|
Primary Outcome
|
|
|
|
Mean DD symptom severity scores
|
PHQ-9 (41) )
|
√
|
|
Secondary Outcomes
|
|
|
|
Mean DD symptom severity scores
|
PHQ-9 (41)
|
|
√
|
Remission (proportion with PHQ-9 scores <5)
|
PHQ-9 (41)
|
√
|
√
|
Mean generalised anxiety disorder (GAD) severity scores
|
GAD-7 (43)
|
√
|
√
|
Quality adjusted life years (QALYs)
|
EQ-5D-5L (44)
|
√
|
√
|
Days out of work (over 3 months)
|
Patient cost questionnaire
|
√
|
√
|
Functional impairment and welfare
|
OxCAP-MH (45)
|
√
|
√
|
Patients’ satisfaction with depression care
|
Modified Patient Satisfaction Survey by Ede et al, 2015 (46)
|
√
|
|
Carers’ perceptions and satisfaction levels with integration efforts at HIV clinic
|
Modified Staff Survey by Ede et al, 2015 (46)
|
√
|
|
Proportion with virological failure (a proxy measure of adherence; defined as a viral load of 400 copies/ml or more)
|
HIV viral load (copies/ml)
|
|
√
|
Reported adherence to ART (proportion of participants who have missed at least one dose of ART in the past three days compared against the baseline value)
|
Assessed by means of the question, ‘Have you missed taking ART in the last 3 days?’ Possible responses 1=Yes, 2=No
|
√
|
√
|
Key: Carer = lay health worker, case manager, mental health workers; ART= antiretroviral therapy
Sample size and power considerations
Power Considerations for Primary Outcome
Twenty clusters will be randomized to each study arm, with the randomisation stratified by type of health facility. The sample size for this trial was calculated using the following assumptions, with testing carried out at the 2.5% significance level for the primary endpoint to allow for multiple testing:
- a) For the mean DD symptom severity score at 3 months
- The within-cluster standard deviation in both arms for the DD combined symptom severity score will be at most 4.4 units (based on the results of the INDEPTH trial in Uganda (47), for screen positive subjects)
- The mean symptom severity score in the CSC arm at 3 months will be 4 units compared to a mean score of 6 units in the EUC arm.
- The harmonic mean of the number of participants per clinic will be 15
- The between cluster coefficient of variation for the PHQ-9 score will be 0.25 in both arms
Using these assumptions and the formula from Hayes and Moulton (48) (page 110 equation 7.9) C= 1 + (zα/2 + zβ)2 {2 σw2 / m + k2 (μ02 + μ1 / (μ0 - μ1 ) (48); where m is the harmonic mean of the number of participants per clinic, k is the between cluster coefficient of variation, σw2 is the within-cluster variance of the DD combined symptom severity scores, μ0 is the mean DD combined symptom severity score at 3 months in the EUC arm and μ1 the combined symptom severity score at 3 months in the CSC arm.
Then a sample size of 20 clusters per arm will give 90% power to detect as statistically significant at the 2.5% level a true mean difference between the EUC and CSC arms of 2 units in the DD symptom severity score.
The sample size calculation is conservative in having used a large estimate of the within cluster standard deviation, as adjusting for baseline DD score is likely to reduce this.
Data collection and management
Data from study participants at baseline, 3 months, and 12 months’ post-enrollment will be collected on printed interviewer-administered face-to-face paper questionnaires which will be stored in lockable filing cabinets at each study site. All the completed questionnaires will be reviewed by a research team member for missing data and unusual responses. Corrective action will be undertaken where necessary by the study research assistant, either by means of a telephone call or by asking the study participant to come back to the clinic. For this, the Data Section of the MRC/UVRI & LSHTM Uganda Research Unit will design a study database in OpenClinica, using unique study identification-number as a linking field. At regular intervals study questionnaires will be retrieved and transferred to the data section of the MRC/UVRI & LSHTM Uganda Research Unit for double data entry. During data entry, the data manager will periodically carry out a set of pre-defined quality checks on the data and raise any queries with the research assistants through the study coordinator. The OpenClinica database will maintain a complete audit trail of the changes made during data cleaning. Once data for a given survey round in the cluster randomised trial has been cleaned and validated, the data will be locked and exported to Stata for statistical analysis. The dedicated data manager assigned to the study will carry out regular quality control checks on the study database. When all of the queries of a given phase of the study, or a given round of the cluster randomized trial have been addressed, the data manager will upload the cleaned data into the main study database. The main study database will be backed up onto a secure location using a mirror server. In addition, the data manager will maintain a password protected copy of the database on his/her computer and on an external hard drive. A detailed data dictionary will be prepared to help with the curation of the data. The master database for the study will be maintained on the server of the Unit. The data manager and study statisticians will also have password protected copies of the master database.
Statistical analysis
Analyses will be conducted on an intention-to-treat (ITT) basis. For the primary outcome of ‘DD symptom severity scores at 3 months’ linear mixed models will be fitted to compare the two treatment arms (CSC and EUC) with terms for treatment arm, stratum (level of health facility) and baseline DD symptom severity score, with a random effect fitted for clinic. A priori moderators will include gender, social class and baseline severity.
For the binary secondary outcome measures, random effects logistic regression models will be fitted with similar terms to those fitted for the DD severity score analysis. Models with multiple time periods will be estimated using ANCOVA assuming low auto-correlation between time periods (49). Exploratory longitudinal analyses will be carried out using three-level multilevel models with the levels being clusters, PLWH within clusters and occasions within PLWH (periods). These models will consider a) the effect of period e.g. whether the symptom score decreases linearly over time and b) whether there is a treatment arm by period interaction i.e. whether the treatment effect reduces or increases over time.
For the cost-effectiveness component of the study, a micro-costing will be performed to obtain the mean cost per patient, the EQ-5D will be used to construct QALYs and a Markov model will be used to predict the outcomes and cost over the lifetime of the patients (49).
Missing data on outcomes and key covariates will be assessed, and if >5% of participants are missing data multiple imputation methods appropriate for multilevel data will be used (50).
Monitoring the trial
Four committees will monitor the progress of the trial, that is, Independent Data Monitoring Committee (IDMC), Trial Steering Committee (TSC), Trial Management Team (TMT) and the Trial Management Group (TMG) and details are shown in appendix 2.
Ethics and dissemination
The protocol was reviewed and approved by the Uganda Virus Research Institute (UVRI) Research and Ethics Committee (reference number GC/127/20/04/772), the Uganda National Council for Science and Technology (reference number HS645ES), and the London School of Hygiene and Tropical Medicine (LSHTM) Ethics Committee (reference number 22567). Any protocol modifications will be submitted to the UVRI Research and Ethics Committee for review, and participants will be informed if warranted. The LSHTM is the trial sponsor. Written (or witnessed if the participant is illiterate) will be mandatory to enrolment. Separate consents will be obtained for storage of blood samples for future studies and as well as used for genetic studies. All participant data will be stored securely and access will be restricted. In order to maintain participant confidentiality, all study data collection forms will only be identified by the study identification numbers. Documents that contain participant’s names such informed consent forms will be stored separately from data collection forms. All databases will be password protected. HIV-infected persons who do not enrol in the study for any reason will be counselled and referred for care. Serious Advance Events (SAEs) (death, suicide attempt, hospitalisation) from any cause will be reported as soon as possible within seven calendar days of becoming aware of SAE to the UVRI Research and Ethics Committee and to the IDMC.
Results produced by this investigation will be presented at local and international conferences and published in a timely fashion, ideally in the last year of the study period. All final peer-reviewed manuscripts that arise from this proposal will be submitted to the digital archive PubMed Central for open access.