221 Background: While post-surgical ctDNA is a known biomarker for risk of recurrence in colon cancer patients (pts), the prognostic value of presurgical ctDNA is less understood. Here, we explore whether presurgical ctDNA levels can predict outcomes and identify colon cancer pts who may benefit from earlier intervention. Methods: This retrospective study analyzed presurgical ctDNA (Signatera) data from 2,517 resectable stage I-IV colon cancer pts who enrolled in GALAXY (UMIN000039205) and did not receive neoadjuvant chemotherapy. The goal was to predict disease-free survival (DFS) by training a random forest classifier with 15 presurgical clinicopathological variables. The cohort was randomly partitioned into a training set (80%, n = 2018) and a test set (20%, n = 499) using stratified sampling to preserve the joint distribution of clinical stage and sex. The training set was used for model fitting and hyperparameter optimization via 5-fold cross-validation. The test set was used to estimate predictive performance. Variable importance was evaluated using permutation-based methods. To stabilize importance estimates, the final model was refitted on the full cohort with tuned hyperparameters. Multivariate ROC models informed the selection of thresholds for grouping patients by mean tumor molecules (MTM)/mL levels (undetectable, 0–1, >1–5, >5–55, and >55 MTM/mL). Finally, the association between ctDNA levels and early relapse (5–55 MTM/mL (HR, 1.70; 95% CI, 1.06–2.7, p=0.028) and >55 MTM/mL (HR, 2.36; 95% CI, 1.38–4.0, p=0.002) had a significantly inferior DFS (36-month DFS: 74.0% and 59.4%, respectively). Among all pts who relapsed (n=482), 37.1% (179/482) relapsed early. Presurgical ctDNA levels across all thresholds were significantly associated with the frequency of pts who experienced early vs. later relapse (p=1e-04), with ctDNA >5 MTM/mL associated with 6x higher odds of early relapse compared to 0 MTM/mL. ACT nearly halved the odds of early relapse (Mantel-Haenszel OR, 0.53; 95% CI, 0.37–0.76, p=0.0005), with 4.8% (47/980) of pts who received ACT relapsing early vs 7.5% (115/1538) of those who did not. Conclusions: Presurgical ctDNA levels in colon cancer pts undergoing upfront surgery may serve as a biomarker for predicting early relapse and poor DFS. Adjuvant chemotherapy significantly reduces the risk of early relapse, supporting further research into the use of longitudinal pre- and post-surgical ctDNA to guide optimal neoadjuvant and adjuvant systemic therapy. Clinical trial information: UMIN000039205 .
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Naoya Akazawa
Saori Mishima
K. Ando
Journal of Clinical Oncology
Kyushu University
Yokohama City University
Aichi Cancer Center
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Akazawa et al. (Sat,) studied this question.
www.synapsesocial.com/papers/6966f2fb13bf7a6f02c00708 — DOI: https://doi.org/10.1200/jco.2026.44.2_suppl.221