Abstract 598P
Background
There is uncertainty whether early closure (EC) of a defunctioning stoma influences the complete administration of the adjuvant chemotherapy (CoC) after low anterior rectal resection (LAR) for rectal cancer. CoC was previously shown in retrospective analyses to improve the five-year OS and DFS.
Methods
CoCStom trial was a prospective randomized multicenter investigator-initiated study. Patients undergoing neoadjuvant therapy (chemoradiation or 5x5 Gy radiotherapy) followed by LAR for locally advanced rectal cancer were randomized in two arms. Experimental - EC, 8 to 10 days after LAR; and control - late closure of the stoma (LC), after completion of the adjuvant chemotherapy (26 weeks) which included both 5-FU- and oxaliplatin-based regimens according to local practice and tumor stage. The primary endpoint was CoC. The study was designed to show an CoC improvement of 20 % (power 80%, alpha-value 0.05). Secondary endpoints: oncological and surgical outcomes as well as quality of life.
Results
A total of 257 patients with comparable baseline characteristics and pathohistological (UICC) stages were randomized between 2013 and 2018. Of these, 233 (EC: 116 vs. LC: 117) were eligible for analysis. Median follow up was 24 months. Surgical morbidity after stoma closure was comparable (Clavien Dindo III-IV: EC vs. LC: 15.8 vs. 18.9%). The median hospitalization after LAR was 17 days in both groups. CoC was similar EC [62.9% (95% CI: 53.5 - 71.7%] and LC [65.8% (56.5 -74.3%]. Patients in the EC group started adjuvant chemotherapy (median 38 vs. 27 days after randomization) significantly later and received less oxaliplatin-based regimens (8.5 vs. 15%). DFS was numerically better in the EC group (HR 1.6; 95% CI: 0.83 – 3.06).
Conclusions
EC of the stoma was feasible and did not lead to increased surgical morbidity. CoC was not improved, however, a trend towards better DFS was observed within the EC group despite similar CoC, a later start of adjuvant therapy as well as less use of oxaliplatin-based regimens. Thus, EC of the stoma appears to be a valid option for patients undergoing LAR.
Clinical trial identification
DRKS00005113.
Editorial acknowledgement
Legal entity responsible for the study
Flavius Sandra-Petrescu, MD, on behalf of the CoCStom Study Group.
Funding
German Research Foundation (DFG) - KI1315/2-1 and SA 3642/1-2.
Disclosure
All authors have declared no conflicts of interest.
Resources from the same session
622P - Evaluation of the metastatic colorectal cancer score (mCCS) in predicting outcome for patients with RAS wild type metastatic colorectal cancer (mCRC) treated with first-line (1L) panitumumab (PAN) plus FOLFIRI/FOLFOX: Updated interim results of the non-interventional study VALIDATE
Presenter: Marcel Reiser
Session: Poster session 10
623P - VIC regimen (vemurafenib/irinotecan/cetuximab) versus bevacizumab plus chemotherapy as first-line treatment for BRAF V600E-mutated advanced colorectal cancer
Presenter: Yijiao Chen
Session: Poster session 10
624P - Tolerability and safety of vemurafenib, cetuximab combined with camrelizumab for BRAF V600E-mutated /MSS metastatic colorectal cancer
Presenter: Meng Qiu
Session: Poster session 10
625P - Efficacy and safety of the combination of encorafenib and cetuximab in patients with BRAF V600E mutated metastatic colorectal cancer: An AGEO real-world multicentre study
Presenter: Claire Gallois
Session: Poster session 10
626P - Mucinous differentiation (MD) as predictor of response in BRAF-V600E mutated metastatic colorectal cancer (mCRC) treated with BRAF inhibitors (BRAFi) combinations
Presenter: Francisco Javier Ros Montana
Session: Poster session 10