What question did this study set out to answer?

This research aims to identify factors influencing patient participation in clinical trials for renal cell carcinoma and urothelial carcinoma.

March 4, 2026

Patient and trial design factors influencing participation in prospective bladder and kidney cancer clinical trials.

Key Points

This research aims to identify factors influencing patient participation in clinical trials for renal cell carcinoma and urothelial carcinoma.
Retrospective review of patients referred to a uro-oncology centre from January 2020 to December 2022.
Assessment of associations between consent and patient characteristics (age, gender, ethnicity) and trial features (randomisation, phase).
Classification of reasons for non-screening into categories like patient preference and performance status.
Use of multivariable logistic regression analysis to identify independent predictors of screening initiation.
406 patients were included, with 217 having RCC and 189 with UC.
Older age and non-white ethnicity correlated with lower consent rates.
34% of patients cited preference as a reason for not participating, higher in non-white patients (31%).
Participation was lower in randomised trials (48.1%) compared to non-randomised (73.7%) with a p-value of 0.032.
Higher consent was observed in early phase trials (86%) versus phase 3 (42.6%), but this was not an independent predictor in the analysis.

Abstract

655 Background: Patients on clinical trials with renal cell carcinoma (RCC) or urothelial carcinoma (UC) have better outcomes than those receiving standard of care. However, some patients choose not to participate in trials. Overrepresentation of certain groups can bias trial results. Here, we explore the characteristics of patients who decline participation in RCC and UC trials. Methods: We retrospectively reviewed patients with RCC or UC who were referred to a single uro-oncology cancer centre, St Bartholomew’s Hospital, between January 2020 and December 2022. Each patient was followed until October 2024. We assessed associations between consent and patient characteristics (age, gender, ethnicity) and trial characteristics (randomisation, phase, comparator: placebo vs active treatment). Reasons for not starting screening were classified as patient preference, performance status, comorbidities, histology or others. Independent predictors of screening initiation were identified using multivariable logistic regression analysis (MVA). Results: A total of 406 patients (189 UC, 217 RCC) were included. Older age and non-white ethnicity were associated with lower consent rates (Table 1). Patient preference was the most common reason for non-screening (34% overall, 31% among non-white patients). Trial design characteristics also had an impact, with lower participation in randomised trials (48.1%) compared to non-randomised (73.7%) (p=0.032). The presence of a placebo arm was not significant in the MVA (p=0.293). Consent was higher in early phase than late phase trials on univariable analysis (p<0.001), with lower rates in phase 3 (42.6%) compared to early phase trials (86%). However, it was not an independent predictor in the MVA. Conclusions: Specific trial and patient characteristics predispose to non-clinical trial participation. Addressing these factors may result in a more broadly representative patient population in clinical trials. Multivariable logistic regression analysis. Variable OR 95% CI p value Age 0.96 0.93-0.98 0.0008 Ethnicity 0.27 0.11-0.63 0.0028 Randomisation 0.33 0.11-0.94 0.032 Phase 1 and 2 1.64e-7 1e-170 – 5e7 0.987 Phase 3 1.2e-8 NA – 7.4e20 0.985 Active treatment 1.80 0.02-1.56 0.127 Placebo 1.09 0.04-2.50 0.293

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Patient and trial design factors influencing participation in prospective bladder and kidney cancer clinical trials.

Key Points

Abstract

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