What question did this study set out to answer?

This research aims to evaluate how clinical staging impacts disease-free survival (DFS) in renal cell carcinoma, optimizing future neoadjuvant trial designs.

May 29, 2026

Relationships between clinical stage, pathological stage, and disease-free (DFS) survival in renal cell carcinoma as used to inform future neoadjuvant study design: ECOG-ACRIN EA8143 PROSPER analysis.

Key Points

This research aims to evaluate how clinical staging impacts disease-free survival (DFS) in renal cell carcinoma, optimizing future neoadjuvant trial designs.
Randomized patients with renal cell carcinoma were assigned to presurgical nivolumab or surgery alone.
Disease-free survival analysis was conducted on clinical stages, tumor sizes, and transitions from clinical to pathological stages.
Cox proportional hazards models and log-rank tests were employed to analyze DFS outcomes.
Overall, DFS was significantly better for cT1/cT2 versus cT3/cT4 patients (HR=1.56, p<0.001).
In the cT3a group, DFS was worse for patients with tumors >8cm compared to those <7cm (HR=3.33, p<0.001).
About 50% of cT1/T2 patients were upstaged to pT3/4, highlighting significant pathological upstaging risks.

Abstract

4540 Background: Estimating risk of renal cell cancer (RCC) relapse based only on pre-surgical data is key to future neoadjuvant trial design. The EA PROSPER phase 3 study accrued pts with clinical stage ≥T2 or T any N+ RCC of any histology for nephrectomy. Pts were randomized to presurgical nivolumab (nivo) followed by primary tumor resection and 9 cycles of adjuvant nivo, or surgery alone followed by observation. We used PROSPER data to assess how baseline data informs risk. We reviewed cT to pT stage transitions, associated cT stages with outcome, and asked if size in addition to cT stage increases predictive accuracy. Methods: Pts with clear cell (cc) RCC were included. cT to pT concordance was assessed by TNM 8 th edition. DFS analysis (time from surgery to recurrence, second primary, or any cause death) was performed; pts with no event were censored at date of last assessment. DFS analysis compared cT groups (cT1/cT2 vs cT3/cT4) in the overall eligible study population and within each study arm. A subset DFS analysis by tumor size among cT2a (> 7-8cm vs >8-10cm) and cT3a ( 8cm) was explored. Cox proportional hazards models were used, and log-rank test was reported to represent global p-value of each model. Wald test p-value was reported for individual group comparison (in assessing more than two groups). Two-sided p-values are reported, all p-values were considered significant at 0.05. Results: Of 819 pts randomized, 732 ccRCC pts (382 surgery only, 350 nivo + surgery) had data available. DFS was significantly different between cT1/cT2 vs. cT3/cT4 group, favoring cT1/cT2 among all pts (HR cT1/cT2 as reference=1.56, two-sided log-rank p 8cm groups when compared to 8cm vs 8cm. Conclusions: In ccRCC pts, baseline cT assessment is associated with DFS outcome. High grade cT1/2 pts risk pathological upstaging to pT3. cT3+ identifies high risk pts, with 8cm have a worse prognosis than patients with < 7cm tumors. These findings should be accounted for in eligibility criteria and risk assessment models for neoadjuvant trials, and explored in other international datasets.

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Cite This Study

Jones et al. (Wed,) studied this question.

synapsesocial.com/papers/6a192d2efab5b468c44160ef https://doi.org/https://doi.org/10.1200/jco.2026.44.16_suppl.4540

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