SENECA study: staging endometrial cancer based on molecular classification

Author:

Chacon EnriqueORCID,Boria FelixORCID,Lyer R RajagopalanORCID,Fanfani Francesco,Malzoni Mario,Bretová PetraORCID,Luzarraga Aznar AnaORCID,Fruscio RobertORCID,Jedryka Marcin AORCID,Tóth RichardORCID,Perrone Anna MyriamORCID,Kakkos Athanasios,Cristóbal Quevedo IgnacioORCID,Congedo Luigi,Zanagnolo Vanna,Fernandez-Gonzalez SergiORCID,Ferro Beatriz,Narducci Fabrice,Hovhannisyan Tatevik,Aksahin Elif,Cardenas Laura,Oliver M Reyes,Nozaleda Gonzalo,Arnaez MartaORCID,Misiek Marcin,Ferrero Annamaria,Pain Flore Anne,Zarragoitia Janire,Diaz Cristina,Ceppi Lorenzo,Mehdiyev Shamsi,Roldán-Rivas Fernando,Guijarro-Campillo Alberto RafaelORCID,Amengual JoanaORCID,Manzour NabilORCID,Sanchez Lorenzo LuisaORCID,Núñez-Córdoba Jorge M,Gonzalez Martin AntonioORCID,Minguez Jose AngelORCID,Chiva LuisORCID

Abstract

ObjectiveManagement of endometrial cancer is advancing, with accurate staging crucial for guiding treatment decisions. Understanding sentinel lymph node (SLN) involvement rates across molecular subgroups is essential. To evaluate SLN involvement in early-stage (International Federation of Gynecology and Obstetrics 2009 I–II) endometrial cancer, considering molecular subtypes and new European Society of Gynaecological Oncology (ESGO) risk classification.MethodsThe SENECA study retrospectively reviewed data from 2139 women with stage I–II endometrial cancer across 66 centers in 16 countries. Patients underwent surgery with SLN assessment following ESGO guidelines between January 2021 and December 2022. Molecular analysis was performed on pre-operative biopsies or hysterectomy specimens.ResultsAmong the 2139 patients, the molecular subgroups were as follows: 272 (12.7%) p53 abnormal (p53abn, 1191 (55.7%) non-specific molecular profile (NSMP), 581 (27.2%) mismatch repair deficient (MMRd), 95 (4.4%) POLE mutated (POLE-mut). Tracer diffusion was detected in, at least one side, in 97.2% of the cases; with a bilateral diffusion observed in 82.7% of the cases. By ultrastaging (90.7% of the cases) or one-step nucleic acid amplification (198 (9.3%) of the cases), 205 patients were identified with affected sentinel lymph nodes, representing 9.6% of the sample. Of these, 139 (67.8%) had low-volume metastases (including micrometastases, 42.9%; and isolated tumor cells, 24.9%) while 66 (32.2%) had macrometastases. Significant differences in SLN involvement were observed between molecular subtypes, with p53abn and MMRd groups having the highest rates (12.50% and 12.40%, respectively) compared with NSMP (7.80%) and POLE-mut (6.30%), (p=0.004); (p53abn, OR=1.69 (95% CI 1.11 to 2.56), p=0.014; MMRd, OR=1.67 (95% CI 1.21 to 2.31), p=0.002). Differences were also noted among ESGO risk groups (2.84% for low-risk patients, 6.62% for intermediate-risk patients, 21.63% for high–intermediate risk patients, and 22.51% for high-risk patients; p<0.001).ConclusionsOur study reveals significant differences in SLN involvement among patients with early-stage endometrial cancer based on molecular subtypes. This underscores the importance of considering molecular characteristics for accurate staging and optimal management decisions.

Publisher

BMJ

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