# PLAN-psoriasis: protocol for a randomised controlled feasibility trial comparing patient-led ‘as-needed’ treatment and therapeutic drug monitoring-guided treatment to continuous treatment for adults with clear or almost clear skin on risankizumab monotherapy for psoriasis

**Authors:** Weiyu Ye, Kingsley Powell, Niamh Dooley, Charlotte M Thomas, Bola Coker, Helen McAteer, Jessica Ruoheng Wei, Wei Ren Tan, David Baudry, Tejus Dasandi, Jade Pizzato, Tracey H Sach, John Gregory, Zijing Yang, Andrew E Pink, Richard T Woolf, Richard B Warren, John Weinman, Jonathan N Barker, Sarah Chapman, Joseph F Standing, Sam Norton, Catherine H Smith, Satveer K Mahil

PMC · DOI: 10.1136/bmjopen-2025-106635 · 2025-10-10

## TL;DR

This study tests if personalized treatment strategies for psoriasis can reduce drug use while maintaining skin health, compared to continuous treatment.

## Contribution

The study introduces a feasibility trial comparing patient-led and drug-monitoring guided treatment strategies to standard continuous treatment for psoriasis.

## Key findings

- The trial will assess the practicality and acceptability of personalized dose minimization strategies for psoriasis.
- Healthcare cost and resource data collection feasibility will be evaluated for future cost-effectiveness analysis.
- Qualitative insights from patients and clinicians will inform the design of a future definitive trial.

## Abstract

Targeted biologic therapies have transformed outcomes for individuals with psoriasis, a common immune-mediated inflammatory skin disease. The widespread use of these highly effective treatments has led to a growing number of individuals with clear or nearly clear skin remaining on continuous, long-term treatment. Personalised strategies to minimise drug exposure may sustain long-term disease control while reducing treatment burden, associated risks and healthcare costs. This study aims to evaluate the feasibility of a definitive pragmatic effectiveness trial of two personalised dose minimisation strategies compared with continuous treatment (standard care) in adults with well-controlled psoriasis receiving the exemplar biologic risankizumab.

This is a multicentre, assessor-blind, parallel group, open-label randomised controlled feasibility trial in the UK, evaluating two personalised biologic dose minimisation strategies for psoriasis. 90 adults with both physician-assessed and patient-assessed clear or nearly clear skin on risankizumab monotherapy for ≥12 months will be randomised in a 1:1:1 ratio to (1) patient-led ‘as-needed’ treatment, where risankizumab is administered at the first sign of self-assessed psoriasis recurrence, (2) therapeutic drug monitoring-guided treatment, with personalised dosing intervals determined using a pharmacokinetic model or (3) continuous treatment as per standard care, for 12 months. Participants will be invited to submit self-reported outcomes and self-taken photographs every 3 months using a bespoke remote monitoring system (mySkin app) and will attend an in-person assessment at 12 months. They may also request additional patient-initiated follow-up appointments during the trial if needed. The primary outcome is the practicality and acceptability of the two personalised biologic dose minimisation strategies, assessed as a composite measure including recruitment and retention rates, adherence to the assigned strategies and acceptability to both patients and clinicians. The feasibility of collecting healthcare cost and resource utilisation data will also be evaluated to inform a future cost-effectiveness analysis. A nested qualitative study, involving semistructured interviews with patients and clinicians, will explore perspectives on the personalised biologic dose minimisation strategies. These findings will inform the design of a future definitive trial.

This study received ethical approval from the Seasonal Research Ethics Committee (reference 24/LO/0089). Results will be disseminated through scientific conferences, peer-reviewed publications and patient/public engagement events. Lay summaries and infographics will be codeveloped with patient partners to ensure the findings are accessible for the wider public.

ISRCTN17922845.

## Linked entities

- **Diseases:** psoriasis (MONDO:0005083)

## Full-text entities

- **Diseases:** psoriasis (MESH:D011565), inflammatory skin disease (MESH:D012871)
- **Chemicals:** risankizumab (MESH:C000601773)
- **Species:** Homo sapiens (human, species) [taxon 9606]

## Figures

2 figures with captions in the complete paper: https://tomesphere.com/paper/PMC12519699/full.md

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Source: https://tomesphere.com/paper/PMC12519699