TY - JOUR
T1 - External multicentre validation of pseudomyxoma peritonei PSOGI-Ki67 classification
AU - EuroPMP COST action and GECOP group
AU - Arjona-Sanchez, A.
AU - Martinez-López, A.
AU - Moreno-Montilla, M. T.
AU - Mulsow, J.
AU - Lozano-Lominchar, P.
AU - Martínez-Torres, B.
AU - Rau, B.
AU - Canbay, E.
AU - Sommariva, A.
AU - Milione, M.
AU - Deraco, M.
AU - Sgarbura, O.
AU - Torgunrud, A.
AU - Kepenekian, V.
AU - Carr, N. J.
AU - Hoorens, A.
AU - Delhorme, J. B.
AU - Wernert, R.
AU - Goere, D.
AU - Martin-Roman, L.
AU - Cosyns, S.
AU - Flatmark, K.
AU - Davidson, B.
AU - Khellaf, L.
AU - Pereira-Perez, F.
AU - Rodriguez-Ortiz, L.
AU - Ibáñez-Costa, A.
AU - Romero-Ruiz, A.
AU - Rufián-Andújar, B.
AU - Valenzuela-Molina, F.
AU - Casado-Adam, A.
AU - Sánchez-Hidalgo, J. M.
AU - Rufián-Peña, S.
AU - Ortega-Salas, R.
AU - Granados-Rodríguez, M.
AU - Vázquez-Borrego, M. C.
AU - Bura, F. I.
AU - Castaño, J. P.
AU - Kusamura, S.
AU - Baratti, D.
AU - Guaglio, M.
AU - Angel Castaño, Pascual A.
AU - de Valbuena Bueno C, Ruiz
AU - Quénet, F.
AU - Yilmaz, S.
AU - Canbay, Torun B.
AU - Sola Vendrell, E.
AU - González-Bayón, L.
AU - Ceelen, W.
AU - Honore, Charles
N1 - Publisher Copyright:
© 2023 Elsevier Ltd, BASO ~ The Association for Cancer Surgery, and the European Society of Surgical Oncology
PY - 2023/8/1
Y1 - 2023/8/1
N2 - Background: Pseudomyxoma peritonei (PMP) is a rare malignant disease. Adding of the Ki67 proliferation index to the PSOGI PMP classification provided two different subcategories of the extensive HG-PMP group (HG-PMP ≤15% and HG-PMP >15%) with different survival in a previous unicentric study. This study aims to carry out an external and multicentre validation of this new proposed classification. Method: It was a prospective analysis of samples from a historical and international cohort of patients. A representative area with higher cellular density was used to determine the Ki67%. The Ki67 proliferation index (%) was determined in all the HG-PMP patients. A Cox proportional hazard models and multivariable COX models were used. The Kaplan–Meier method and the two-tailed log-rank test were used to analyse the effect of different PSOGI-Ki67 categories on OS and DFS. Its predictive accuracy was analysed using Harrel's C-index and the ROC curve. The calibration was performed using the calibration plots matching. Results: After exclusions, 349 patients were available for analysis. The 5-years OS were 86% for LG-PMP, 59% for HG-PMP≤15, 38% for HG-PMP>15 and 42% for SRC-PMP (p = 0.0001). The 5-years DFS were 49% for LG-PMP, 35% for HG-PMP≤15, 16% for HG-PMP>15 and 18% SRC-PMP (p = 0.0001). The discrimination capability of PSOGI-Ki67 was validated. Conclusion: the PSOGI-Ki67 classification discriminates and predicts the OS and DFS in patients with PMP dividing the HG-PMP category into two well-defined sub-categories. The Ki67 proliferation index should be incorporated routinely in the pathology report for these patients.
AB - Background: Pseudomyxoma peritonei (PMP) is a rare malignant disease. Adding of the Ki67 proliferation index to the PSOGI PMP classification provided two different subcategories of the extensive HG-PMP group (HG-PMP ≤15% and HG-PMP >15%) with different survival in a previous unicentric study. This study aims to carry out an external and multicentre validation of this new proposed classification. Method: It was a prospective analysis of samples from a historical and international cohort of patients. A representative area with higher cellular density was used to determine the Ki67%. The Ki67 proliferation index (%) was determined in all the HG-PMP patients. A Cox proportional hazard models and multivariable COX models were used. The Kaplan–Meier method and the two-tailed log-rank test were used to analyse the effect of different PSOGI-Ki67 categories on OS and DFS. Its predictive accuracy was analysed using Harrel's C-index and the ROC curve. The calibration was performed using the calibration plots matching. Results: After exclusions, 349 patients were available for analysis. The 5-years OS were 86% for LG-PMP, 59% for HG-PMP≤15, 38% for HG-PMP>15 and 42% for SRC-PMP (p = 0.0001). The 5-years DFS were 49% for LG-PMP, 35% for HG-PMP≤15, 16% for HG-PMP>15 and 18% SRC-PMP (p = 0.0001). The discrimination capability of PSOGI-Ki67 was validated. Conclusion: the PSOGI-Ki67 classification discriminates and predicts the OS and DFS in patients with PMP dividing the HG-PMP category into two well-defined sub-categories. The Ki67 proliferation index should be incorporated routinely in the pathology report for these patients.
UR - http://www.scopus.com/inward/record.url?scp=85150308268&partnerID=8YFLogxK
U2 - 10.1016/j.ejso.2023.03.206
DO - 10.1016/j.ejso.2023.03.206
M3 - Article
AN - SCOPUS:85150308268
SN - 0748-7983
VL - 49
SP - 1481
EP - 1488
JO - European Journal of Surgical Oncology
JF - European Journal of Surgical Oncology
IS - 8
ER -