Model structure

The schizophrenia WDM simulates the entire disease and treatment pathways for people at clinical high risk of psychoses (CHR) or with a diagnosis of psychosis or schizophrenia over a lifetime horizon. Patients enter the model following referral to secondary mental healthcare services for possible psychosis, and exit the model when they die. A discrete event simulation model was developed with SIMUL8 software (Simul8 Corporation, Glasgow, UK, professional version 15.0 for Windows; see https://www.simul8.com/online/). Discrete event simulation is a modelling method that simulates the experience of each individual patient. The clinical course of each patient is determined based on their characteristics, such as age, family history, previous events (e.g. relapses) and previous treatments.

The structure of the schizophrenia WDM is presented in Fig. 1. There are four modules within the WDM: specialist assessment pathway (module A), CHR pathway (module B), psychosis pathway (module C) and out-of-scope and death pathway (module D).

Fig. 1 Model structure. CBT, cognitive–behavioural therapy; CHR, clinical high risk of psychosis; FEP, first-episode psychosis.

After entering the model through module A, patients are triaged to different modules based on the assessment results: CHR (module B), psychosis (module C) or not at risk of psychosis (module D). Patients at module B can move to module D (if they die) or module C (if they develop psychosis). Patients at module C cannot move to module B, but they can move to module D if they receive a non-schizophrenia diagnosis or die. Patients at module D cannot move to other modules. Within each module, the intervention received by specific patients depends on three factors: their disease status (not at risk of psychosis, CHR, first-episode psychosis (FEP), subsequent acute psychosis or subsequent non-acute psychosis), availability of the intervention and patients’ acceptance of non-compulsory interventions. In the model, it is assumed that patients may refuse to take up CBT and/or family intervention. The prescription of antipsychotic medications is assumed to be optional for patients with FEP in a stable condition, and is compulsory for all the other patients with psychosis. However, patients might discontinue their prescribed antipsychotic medications for various reasons. In the WDM, discontinuation of antipsychotic medications was modelled, and the primary reason for discontinuing antipsychotic medication were grouped into three mutually exclusive categories: inefficacy, intolerance and non-adherence not otherwise specified. Patients who discontinue their antipsychotic medication because of inefficacy are assumed to experience a relapse, and will be switched to a different antipsychotic medication after their relapses have been managed. Patients who discontinue their antipsychotic medication because of intolerance will be switched to a different antipsychotic medication without experiencing a relapse. Patients who discontinue antipsychotic medication because of non-adherence will no longer take any antipsychotic medication until they experience relapses. After managing relapse, those patients will either return to their previous antipsychotic medication, if this is the first time that they discontinue an oral antipsychotic medication because of non-adherence, or be switched to a long-acting injectable antipsychotic medication, if they have discontinued oral antipsychotic medications more than once. A comprehensive description of the model structure is reported by Jin et al.^{Reference Jin, Tappenden, MacCabe, Robinson and Byford7}

Prioritisation of interventions for modelling

The NICE schizophrenia guideline recommended nine key interventions, including specialist mental health assessment, CBT, family intervention, antipsychotic medication, rapid triage assessment of acute psychosis by the crisis resolution and home treatment team, rapid tranquilisation, monitoring and treatment for coexisting conditions, and occupational and educational interventions.¹ Because of data availability issues and resource constraints to this study, it was not possible to model adherence to all interventions recommended by the NICE schizophrenia guideline. Based on importance and data availability, three interventions were prioritised for evaluation with the model: individual CBT for people at CHR, family interventions for patients with FEP and oral clozapine for patients with TRS. The most common reason for excluding an intervention from this analysis was lack of evidence about the clinical and cost impacts of the intervention. A list of interventions excluded are listed in Supplementary File 1, Section 1 available at https://doi.org/10.1192/bjp.2020.241.

Key impacts of the interventions modelled in the study

For each intervention under assessment, the key impacts modelled in the study, including clinical benefits, clinical harms, cost and cost savings, are reported in Table 1. The impacts modelled in the study were chosen based on importance and data availability, as informed by published literature and expert opinion. Because of lack of evidence about the adverse events of CBT and family interventions, clinical harms were only modelled for antipsychotic medication. Five adverse events were modelled for antipsychotic medications: glucose intolerance, diabetes, weight gain, acute extrapyramidal symptoms and neutropenia.

Table 1 Key impacts of interventions considered in the schizophrenia whole-disease model

CBT, cognitive–behavioural therapy; CHR, clinical high risk of psychosis; FEP, first-episode psychosis; TRS, treatment-resistant schizophrenia; EPS, extrapyramidal symptoms.

Input data

Four types of input data were used in our study: clinical evidence, HRQoL, unit cost and healthcare resource use. A list of input data for the schizophrenia WDM is reported in a previous publication.^{Reference Jin, Tappenden, MacCabe, Robinson and Byford7} The key parameters that are most relevant to this study are reported in Supplementary Table 2; these are briefly summarised below. The current provision of CBT and family intervention were obtained from the Early intervention in Psychosis national audit,² which analysed data submitted by 55 mental health providers in England. A recent systematic review^{Reference Thien and O'Donoghue11} identified two studies that reported duration of delay in initiating clozapine for patients with TRS in the UK. The reported duration of delay ranges from 3.98 years in Howes et al^{Reference Howes, Vergunst, Gee, McGuire, Kapur and Taylor4} to 5 years in Najim et al.^{Reference Najim, Heath and Singh12} The result reported by Howes et al was used in our study, because Howes et al was conducted more recently than Najim et al, and has a larger sample size.^{Reference Howes, Vergunst, Gee, McGuire, Kapur and Taylor4} The clinical efficacy data of CBT, family intervention and CBT were informed by published meta-analyses.^{1,Reference Hutton and Taylor13,Reference Samara, Dold, Gianatsi, Nikolakopoulou, Helfer and Salanti14} HRQoL data were obtained from published systematic reviews.^{1,Reference Fusar-Poli, Rocchetti, Sardella, Avila, Brandizzi and Caverzasi15,Reference Alshowkan, Curtis and White16} Resource quantities were mainly informed by the systematic reviews conducted by the NICE schizophrenia guideline,¹⁷ new evidence identified from rapid literature review conducted for this study and expert opinion where no evidence was identified. All costs were reported in 2016/2017 UK Pound Sterling. Unit costs were obtained from the Unit Costs of Health and Social Care 2017,^{Reference Curtis18} prescription cost analysis (England) 2017¹⁹ and the NHS reference costs 2016–2017.²⁰

Outcomes

The model estimates lifetime costs and lifetime QALYs gained for patients referred to secondary care mental health services for possible psychosis. An annual discount rate of 3.5% was applied to both costs and QALYs.¹⁰ To facilitate comparison between different options, incremental cost-effectiveness ratios (ICERs) and incremental net monetary benefit (NMB) were calculated by using the estimates of costs and QALYs for each option assessed. The ICER is calculated as the difference in cost between two competing options, divided by the difference in QALYs. Cost-effectiveness is usually assessed by comparing an ICER against a reference threshold, which is intended to reflect the opportunity cost of displacing one QALY elsewhere in the health system in order to fund the new intervention. If the ICER falls below that threshold, the intervention might be considered to represent a good use of health resources, whereas if the ICER is above the threshold, the intervention is likely to be considered cost-ineffective. NICE's usual threshold (λ) range for determining cost-effectiveness is £20 000–£30 000 per QALY gained for all interventions, except for life-extending treatments for people who are at the end of their life (defined as <24 months to live with current treatment) or for people with very rare diseases. Incremental NMB is a transformation of the ICER given some value of λ, which thereby reflects the monetary value of any additional QALYs gained, less any additional costs (calculated as ΔQALY×λ−ΔCost).

Sensitivity analysis

Three different types of sensitivity analyses were conducted to test the robustness of our results under different input data and/or assumptions: one-way sensitivity analysis, which assesses the impact of changing the value of individual parameter; structural sensitivity analysis, which assesses the impact of using alternative assumptions of the model (e.g. whether CBT can prevent psychosis or whether its effect is limited to delaying the transition from CHR to psychosis); and probabilistic sensitivity analysis (PSA), which assesses the joint impact of changing multiple input data simultaneously. In a PSA, each uncertain parameter is represented using a pre-defined probability distribution. Using Monte-Carlo sampling methods, each model run draws a random sample from each uncertain parameter distribution. For this study, the process was repeated 5000 times, resulting in a distribution of cost and health outputs.