Abstract
BackgroundAdjuvant chemotherapy reduces the risk of recurrence of stage III colon cancer (CC). However, more effective prognostic and predictive biomarkers are needed for better treatment stratification of affected patients. Here, we constructed a 55-gene classifier (55GC) and investigated its utility for classifying patients with stage III CC.MethodsWe retrospectively identified patients aged 20–79 years, with stage III CC, who received adjuvant chemotherapy with or without oxaliplatin, between the years 2009 and 2012.ResultsAmong 938 eligible patients, 203 and 201 patients who received adjuvant chemotherapy with and without oxaliplatin, respectively, were selected by propensity score matching. Of these, 95 patients from each group were analyzed, and their 5-year relapse-free survival (RFS) rates with and without oxaliplatin were 73.7 and 77.1%, respectively. The hazard ratios for 5-year RFS following adjuvant chemotherapy (fluoropyrimidine), with and without oxaliplatin, were 1.241 (95% CI, 0.465–3.308; P = 0.67) and 0.791 (95% CI, 0.329–1.901; P = 0.60), respectively. Stratification using the 55GC revealed that 52 (27.3%), 78 (41.1%), and 60 (31.6%) patients had microsatellite instability (MSI)-like, chromosomal instability (CIN)-like, and stromal subtypes, respectively. The 5-year RFS rates were 84.3 and 72.0% in patients treated with and without oxaliplatin, respectively, for the MSI-like subtype (HR, 0.495; 95% CI, 0.145–1.692; P = 0.25). No differences in RFS rates were noted in the CIN-like or stromal subtypes. Stratification by cancer sidedness for each subtype showed improved RFS only in patients with left-sided primary cancer treated with oxaliplatin for the MSI-like subtype (P = 0.007). The 5-year RFS rates of the MSI-like subtype in left-sided cancer patients were 100 and 53.9% with and without oxaliplatin, respectively.ConclusionsSubclassification using 55GC and tumor sidedness revealed increased RFS in patients within the MSI-like subtype with stage III left-sided CC treated with fluoropyrimidine and oxaliplatin compared to those treated without oxaliplatin. However, the predictive power of 55GC subtyping alone did not reach statistical significance in this cohort, warranting larger prospective studies.Trial registrationThe study protocol was registered in the University Hospital Medical Education Network (UMIN) clinical trial registry (UMIN study ID: 000023879).
Highlights
Adjuvant chemotherapy reduces the risk of recurrence of stage III colon cancer (CC)
There were more patients with T4 stage cancer in the cohort treated with oxaliplatin (44/95 patients, 46.3%) than in the cohort treated without oxaliplatin (34/95 patients, 35.8%) (P = 0.022)
There were more patients with < 12 resected lymph nodes in the cohort treated with oxaliplatin (15/95 patients, 15.8%) than in the cohort treated without oxaliplatin (5/95 patients, 5.3%) (P = 0.018)
Summary
Adjuvant chemotherapy reduces the risk of recurrence of stage III colon cancer (CC). More effective prognostic and predictive biomarkers are needed for better treatment stratification of affected patients. We constructed a 55-gene classifier (55GC) and investigated its utility for classifying patients with stage III CC. Adjuvant chemotherapy in stage III colon cancer (CC) after curative intent resection prolongs survival and reduces the risk of tumor recurrence [2]. Emerging data have led to a debate over the optimal duration of chemotherapy, in the context of increased toxicity [3]. Subclassification of stage III CC is an ongoing process based on accumulating patient survival data and features of cancer presentation [4]. Better prognostic and predictive biomarkers are required to stratify patients for adjuvant therapies based on chemotherapy regimen and duration
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