Prognostic value of isolated peritoneal versus other metastatic sites in colorectal cancer (CRC) patients treated by systemic chemotherapy: Findings from 9,265 pts in the ARCAD database.

Author:

Franko Jan1,Shi Qian2,Meyers Jeffrey P.2,Heinemann Volker3,Falcone Alfredo4,Tebbutt Niall C.5,Maughan Tim6,Seymour Matthew7,Saltz Leonard8,Tournigand Christophe9,Diaz-Rubio Eduardo10,Sougklakos Ioannis11,Chibaudel Benoist12,Moen Joseph13,De Gramont Aimery14,Adams Richard A.15,Sargent Daniel J.2,Grothey Axel2

Affiliation:

1. Mercy Medical Center, Des Moines, IA

2. Mayo Clinic, Rochester, MN

3. Department of Internal Medicine III and Comprehensive Cancer Center, Klinikum Grosshadern, Ludwig-Maximilians University of Munich, Munich, Germany

4. Oncology Unit II, University Hospital of Pisa, Pisa, Italy

5. Austin Health, Melbourne, Australia

6. University of Oxford, Oxford, United Kingdom

7. Gastrointestinal Cancer Research Unit, Cookridge Hospital, Leeds, United Kingdom

8. Memorial Sloan Kettering Cancer Center, New York, NY

9. Hopital Henri Mondor, Creteil, France

10. Hospital Clinico San Carlos, Madrid, Spain

11. University of Heraklion, Heraklion, Greece

12. Franco-British Hospital Institute, Levallois-Perret, France

13. Department of Biostatistics, Iowa City, IA

14. Franco-British Institute, Levallois-Perret, France

15. Velindre Hospital NHS Foundation Trust, Cardiff, United Kingdom

Abstract

656 Background: Patients (pts) with peritoneal metastases from CRC (pmCRC) have reduced OS compared to mCRC pts without peritoneal involvement. Here we further investigated the impact of number and location of metastases among pts receiving first-line systemic chemotherapy. Methods: Individual patient data were available on 9,265 pts (median age 64; 63% male; 93% ECOG PS 0-1; 68% colon primary tumor; brain metastases excluded) enrolled onto 12 first-line randomized trials (4 tested targeted regimens). Stratified multivariable Cox models were used to assess the associations with overall survival (OS); adjusted hazard ratios (HRadj) and 95% confidence intervals are reported (CI). Results: There were 7,963 (86%) pts with non-pmCRC (3,904 with one disease site; 4,059 with ≥2 disease sites), 191 (2%) pts with isolated pmCRC, and 1,111 (12%) non-isolated pmCRC. These groups were similar in age, race, and use of targeted chemotherapy. Compared to non-pmCRC, pts with pmCRC were more likely to be female (41% vs. 36%, p<.001), have colon primary tumors (85% vs. 67%, p<.0001), and have PS2 (10% vs. 6%, p<.0001). Compared to isolated pmCRC, pts with solitary non-peritoneal sites (both M1a) had significantly better OS (HRadj=0.78; CI, 0.64-0.94, p=.009) while pts with ≥2 non-peritoneal sites had similar OS (HRadj=1.06; CI 0.88-1.28, p=.535). OS of pts with pmCRC with a single other disease site (n=446) was similar to isolated pmCRC (HRadj=1.13; CI 0.91-1.40, p=.28), but those with pmCRC + ≥2 additional disease sites (n=665) had shortest survival (HRadj=1.44; CI 1.17-1.77, p<.001). A combination of peritoneal and liver metastases (n=821; HRadj=1.37, CI 1.12-1.67, p=.002) was associated with poorer survival compared with isolated pmCRC; but combination with extrahepatic sites (n=290; HRadj=1.15, CI 0.91-1.45, p=.25) was not. Conclusions: pmCRC pts have significantly worse survival than those with other solitary site mCRC. Among those with multiple disease sites, poorer survival is a function of increased number of metastatic sites and peritoneal involvement, which indicates prognostic heterogeneities among M1b pts.

Publisher

American Society of Clinical Oncology (ASCO)

Subject

Cancer Research,Oncology

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