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. Author manuscript; available in PMC: 2020 Apr 1.
Published in final edited form as: Clin Cancer Res. 2019 Jun 20;25(19):5843–5851. doi: 10.1158/1078-0432.CCR-19-0863

Table 2.

Multivariable Cox proportional hazards model analysis for OS and RFS in 490 patients*

Factor No. of patients No. of events Multivariable HR 95% CI P value
OS
Gene mutation
BRAF 10 6 2.95 1.27–6.86 0.012
RAS 249 87 2.14 1.53–2.99 < 0.001
TP53 347 123 2.21 1.49–3.28 < 0.001
SMAD4 55 25 1.82 1.17–2.83 0.008
Clinicopathologic factors
 Largest liver metastasis diameter 1.07 1.01–1.13 0.033
 Surgical margin, positive 97 33 1.83 1.23–2.72 0.003
RFS
Gene mutation
RAS 249 206 1.47 1.20–1.82 < 0.001
TP53 347 283 1.40 1.11–1.78 0.005
SMAD4 55 51 1.62 1.20–2.20 0.002
Patients factors
 Age 1.01 1.00–1.02 0.024
Clinicopathologic factors
 Number of CLM 1.04 1.01–1.07 0.006
 Largest liver metastasis diameter 1.08 1.04–1.13 < 0.001
 Prehepatectomy chemotherapy 134 117 1.45 1.16–1.82 0.001
 Extrahepatic disease 79 74 1.70 1.31–2.21 < 0.001
 Surgical margin, positive 97 80 1.43 1.11–1.85 0.006

Abbreviations: HR, hazard ratio; CI, confidence interval, CLM, colorectal liver metastasis.

*

Of the 507 patients, 490 patients were analysed because data were unavailable for T category in 8 patients and lymph node metastasis in 14 patients.

The Cox proportional hazards model analysis initially included age (continuous variable), sex, primary tumor location, T category, primary lymph node metastasis, prehepatectomy carcinoembryonic antigen level (continuous variable), timing of metastasis (synchronous vs. metachronous), prehepatectomy chemotherapy, extrahepatic disease, number of CLM (continuous variable), largest liver metastasis diameter (continuous variable), surgical margin status (R1 vs. R0), BRAF mutation, RAS mutation, TP53 mutation, APC mutation, PIK3CA mutation, and SMAD4 mutation. A backward elimination with a threshold P value of 0.05 was used to select variables for the final models.

> 6 cycles vs. ≤ 6 cycles or no prehepatectomy chemotherapy.