Study design

We conducted this unmasked, general practice-based, cluster randomised, controlled open-label superiority trial across four regions in England, UK, with a cluster defined as a general practice.

The trial was delivered according to the protocol,^{Reference Plappert, Hobson-Merrett and Gibbons17} with amendments made to continue trial delivery and follow-up after the start of the COVID-19 pandemic in early 2020. The authors assert that all procedures contributing to this work comply with the ethical standards of the relevant national and institutional committees on human experimentation and with the Helsinki Declaration of 1975, as revised in 2008. All procedures involving human patients were approved by the West Midlands-Edgbaston Research Ethics Committee (reference number 14/WM/0052). Local NHS approvals were obtained before the start of recruitment in each region from 27 February 2018. We had an independent Data Monitoring Committee and Trial Steering Committee, as agreed with the funder. The trial is registered with the ISRCTN Registry (identifier ISRCTN95702682).

Participants

General practices in England were eligible to participate if they were providing care in the participating areas (Birmingham/Solihull, Plymouth, Cornwall, Somerset); had ≥16 patients on their Quality and Outcomes Framework (QOF) register for SMI; and were willing and able to host the intervention. We initially recruited practices in Lancashire, but had to discontinue following changes in services there.

We included people aged ≥18 years registered with participating general practices; diagnosed with schizophrenia, bipolar or other type of psychosis diagnosis; and with evidence of care needs for this diagnosis in the past 2 years, but not currently requiring acute or ongoing secondary multidisciplinary mental healthcare. We aimed for an average of six individuals per practice. We excluded people who could not give informed consent, who needed access to translation services, for whom the general practitioner (GP) believed that it was not in their best interests, who were currently participating in a trial for psychosis, who were receiving secondary care for dementia or intellectual disability, and/or individuals with significant substance or alcohol issues.

Potential participants using secondary care were identified from secondary care records and other potential participants ‘seen only in primary care’ from general practice records. Information packs were posted to potential participants, inviting participation and emphasising how patient researchers were part of the team.^16,18 Those who did not respond were invited to an appointment or could opt out, and were telephoned where possible. Researchers met those interested in participating and obtained written informed consent.

Randomisation and masking

Once all participants in a practice were recruited and baseline data were collected, we assigned the practice to the PARTNERS intervention or care as usual (control) at a 1:1 allocation, using a computer-generated minimisation algorithm, with allocation minimised on geographical area and estimated practice psychosis population size, according to the QOF register. Allocation was undertaken by a Clinical Trials Unit researcher not involved in delivery or analysis of the trial, and communicated to the practice and participants by letter or preferred method of contact.

It was not possible to blind staff in the general practice or the participants because of the nature of the psychosocial intervention. Researchers conducting follow-up assessments were not blinded for logistical reasons, as they were responsible for maintaining relationships with intervention practitioners and general practices. Statisticians were masked to allocation during primary analyses.

Intervention and usual care descriptions

The PARTNERS intervention was developed in line with the Medical Research Council's complex intervention guidance.^{Reference Baker, Gwernan-Jones and Britten14,Reference Gwernan-Jones, Britten and Allard15,Reference Craig, Dieppe, Macintyre, Michie, Nazareth and Petticrew19} The intervention aims to enable contact and ongoing continuity with a mental health worker (a ‘care partner’) based in primary care, who delivers a coaching approach and liaises with primary care and other services. The theoretical basis for benefit is that one or more of multiple diverse mechanisms to improve health or well-being can be triggered and contribute to improved quality of life. The manualised model (available on request) aims to improve emotional, social, mental and physical health outcomes for people with psychosis. Care partners work with participants to develop a shared understanding about current problems and goals, and utilise coaching and motivational techniques with the intention of encouraging participants to be more confident and proactive about their health through developing self-management skills, and achieve personal goals related to their health or other aspects of their lives. Care partners work collaboratively with primary care, secondary care and other organisations. Place and method of contact (face to face, telephone, text) is flexible, starting with fortnightly contact, stepping down to every 3 months for some if agreed, but stepping up, potentially including referral into secondary care, if required.

In the trial, participants received the PARTNERS intervention for up to 12 months, including a 2-month transition period back to usual care. Participants in the intervention group and already under secondary care either had this care paused or the intensity was reduced according to a protocol specific to each NHS provider. Care partners came from a variety of backgrounds, including occupational therapists, social workers, nurses and support workers. They received 2–3 days of initial training, top-up training throughout the study, and supervision. Supervisors included mental health nurses and psychiatrists who received training in the PARTNERS model. The co-chief investigator (R.B.), an accredited GP with a special interest in mental health, provided cover for supervision during periods of illness or absence. Participants allocated to the control arm continued to receive usual care only, either within primary care only or also within secondary care.

Fidelity of the delivery of intervention against the theoretical model was assessed through a comprehensive mixed-methods process evaluation. The proportion of time care partners were in post and numbers of sessions each individual attended with a care partner are reported in this paper.

Outcomes

Participant outcome data were collected at or shortly after consent and at a single follow-up point. Follow-up was originally planned to be 10 months (±1 month) after randomisation of the practice. The anticipated operational problems of following up the high number of individuals recruited in the final month (n = 56) led to a decision to shorten the follow-up period to 9 months (±1 month) for participants recruited at the end of the recruitment window (February 2020). This ensured follow-up completion by December 2020, keeping within the timelines for the research funding.

The primary outcome measure was quality of life as measured by change in score on the participant-reported Manchester Short Assessment of Quality of Life (MANSA) version 2,^{Reference Priebe, Huxley, Knight and Evans20} from baseline to follow-up. This self-complete questionnaire comprises objective and subjective questions across different life domains (work and education, personal finances, leisure activities, social life, living situation, family life, personal safety and health). It was chosen through a consensus stakeholder process because it has shown sensitivity to change in this population, is short and captures important outcomes that the intervention was designed to achieve.

Participant-reported secondary outcomes collected at baseline and follow-up were the Time Use Survey (TUS; assessing time in structured activity),^{Reference Gershuny21} Questionnaire about the Process of Recovery (QPR-15),^{Reference Neil, Kilbride and Pitt22} full and short versions of the Warwick-Edinburgh Mental Wellbeing Scale ((S)WEMWBS),^{Reference Tennant, Hiller and Fishwick23} Brief INSPIRE (a measure of experience of care),^{Reference Williams, Leamy and Bird24} ICEpop CAPability (ICECAP-A; to measure social well-being)^{Reference Flynn, Huynh and Peters25} and the five-level EuroQol five-dimensional (EQ-5D-5L; for health status).^{Reference Brooks26}

Data about mental healthcare service use were collected from secondary care records. Safety outcomes, analysed from the date of practice unmasking (randomisation) through to 10 months after randomisation, were the number of psychiatric hospital admissions, number of in-patient days as a result of psychiatric admission, number of episodes under home treatment (crisis care) and total days under home treatment (crisis care). Details of serious adverse events (e.g. hospital admissions) were also collected after identification during follow-up by researchers and/or practitioners during routine or PARTNERS care.

Statistical analysis

The original recruitment target was 336 participants across approximately 56 general practice clusters, to detect a mean between group difference of 0.45 points^{Reference Priebe, Kelley and Golden27} in the overall MANSA score, with 90% power and two-sided 5% significance level, assuming an s.d. of 0.9, mean of six participants recruited per cluster (general practice), coefficient of variation of cluster size of 0.74, intracluster correlation (ICC) of 0.05, 20% drop-out at the individual participant level and 10% drop-out at the cluster level. The target standardised effect size was therefore 0.5, selected in line with the target effect size in the DIALOG+ trial.^{Reference Priebe, Kelley and Golden27} The protocol included an interim blinded review of the sample size assumptions, including exploring adjusting for the correlation between baseline and follow-up MANSA scores. From the first 39 participants the observed correlation was 0.69 (80% CI 0.56–0.79); we conservatively allowed for a correlation of 0.5 in a revised sample size calculation. Retaining the other underpinning assumptions of the original calculation indicated requiring primary outcome data from 180 participants (recruitment target of 270 participants allowing for drop-out) or 140 participants (recruitment target of 204 participants) to achieve 90% or 80% power, respectively. To adhere to funder-mandated timescales, the revised aim (agreed with the oversight committees) was to recruit 204 participants from approximately 34 general practices.

A detailed statistical analysis plan was approved before locking the trial database.²⁸ All primary analyses followed the modified intention-to-treat principle (i.e. analysis of the complete-case data according to allocated group). Two prespecified sensitivity analyses of the primary outcome were on a per-protocol basis. Analyses of safety outcomes were on the as-treated basis: for safety event/episode analysis, intervention participants were categorised as being ‘treated’ if they had had at least one interaction with their care partner before the date of onset of the episode/serious adverse event. Analyses were undertaken in Stata version 16.0 for Windows (StataCorp LLC, College Station, Texas, USA; https://www.stata.com/) and R version 4.0.3 for Windows (R Core Team, R Foundation for Statistical Computing, Vienna, Austria; https://cran.r-project.org/bin/windows/base/).

The change between baseline and follow-up in the primary outcome of overall MANSA score was analysed with a random effects linear regression model, with cluster-level minimisation factors (region and practice size) and individual-level baseline overall MANSA score included as fixed effects covariates, and general practice as a random effect. Prespecified sensitivity analyses of the primary outcome assessed the robustness of the primary analysis: (a) per-protocol analysis of participants with follow-up data within their prespecified window; (b) per-protocol analysis to assess the impact of availability of care partner to deliver the intervention, excluding practices where a care partner was available <70% of time; (c) using multiple imputation to assess the effect of missing primary outcome data, including the number of care partner interactions as an auxiliary variable; and (d) complier-average causal effect analyses using two prespecified definitions of fidelity (attendance at a minimum of six care partner sessions, either face to face, by telephone or virtually, with each session lasting a minimum of 10 min; and attendance at a minimum of four care partner sessions during which goals were discussed).

To explore the effects of the COVID-19 pandemic, participants were categorised according to whether their follow-up data was collected before or during the pandemic, with three additional prespecified sensitivity analyses for both the primary outcome and the secondary outcome TUS: (a) separate models for participants providing follow-up data before and after the start of the first UK lockdown, (b) adding an interaction term of allocated group/COVID-19-affected categorisation to the primary analysis model and (c) adding the COVID-19-affected categorisation covariate as an adjustment to the primary analysis model. We also undertook four planned subgroup analyses (region, practice size (small versus large), diagnostic group (bipolar disorder versus schizophrenia or other psychosis) and usual care provider at screening (primary versus secondary care)) of the primary outcome by including the interaction effect of allocated group and the subgroup in separate regression models. All fully adjusted sensitivity and subgroup analyses included the minimisation factors, general practice as a random effect and controlled for the corresponding baseline score.

We analysed continuous secondary outcomes with similar random effects linear regression modelling. Two identified outliers were removed from the analyses of the TUS. We were unable to complete the planned analysis of the number of healthcare monitoring outcomes because of limited availability of data (primary care notes reviews were carried out for 32 participants). After discussion with the oversight committees, no inferential analyses were undertaken of the Brief INSPIRE because of both the levels and patterns of missing data at both baseline and follow-up. No inferential analyses were planned/undertaken of the lifestyle outcomes.