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Oncological outcomes after a pathological complete response following total neoadjuvant therapy or chemoradiotherapy for high-risk locally advanced rectal cancer in the RAPIDO trial. | LitMetric

AI Article Synopsis

  • A study examined the effects of total neo-adjuvant therapy (TNT) compared to standard care (CRT) in rectal cancer patients, focusing on the rates of pathological complete response (pCR) and overall outcomes.
  • Results showed that TNT led to a higher pCR rate (28%) compared to CRT (14%), but both treatment groups had similar 5-year recurrence and survival rates after achieving pCR.
  • Factors linked to a successful pCR included receiving the experimental treatment, having normal pre-treatment carcinoembryonic antigen levels, smaller tumor size, and specific tumor stage, with no increase in pCR rates seen with longer treatment durations.

Article Abstract

Background: A pathological complete response (pCR) following chemoradiation (CRT) or short-course radiotherapy (scRT) leads to a favourable prognosis in patients with rectal cancer. Total neo-adjuvant therapy (TNT) doubles the pCR rate, but it is unknown whether oncological outcomes remain favourable and whether the same characteristics are associated with pCR as after CRT.

Methods: Comparison between patients with pCR in the RAPIDO trial in the experimental [EXP] (scRT, chemotherapy, surgery, as TNT) and standard-of-care treatment [STD] (CRT, surgery, postoperative chemotherapy depending on hospital policy) groups. Primary and secondary outcomes were time-to-recurrence (TTR), overall survival (OS) and association between patient, tumour, and treatment characteristics and pCR.

Results: Among patients with a resection within six months after preoperative treatment, 120/423 (28%) [EXP] and 57/398 (14%) [STD] achieved a pCR. Following pCR, 5-year cumulative TTR and OS rates in the EXP and STD arms were 8% vs. 7% (hazard ratio 1.04, 95%CI 0.32-3.38) and 94% vs. 93% (hazard ratio 1.41, 95%CI 0.51-3.92), respectively. Besides the EXP treatment (odds ratio 2.70, 95%CI 1.83-3.97), pre-treatment carcinoembryonic antigen (CEA) <5, pre-treatment tumour size <40 mm and cT2 were associated with pCR. Distance from the anal verge was the only characteristic with a statistically significant difference in association with pCR between the EXP and STD treatment (P=0.042). pCR rates did not increase with prolonged treatment time.

Conclusions: The doubled pCR rate of TNT compared to CRT results in similar oncological outcomes. Characteristics associated with pCR are the EXP treatment, normal CEA, and small tumour size.

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Source
http://dx.doi.org/10.1016/j.ejca.2024.114044DOI Listing

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