ESTRO 2023

Session Item

Sunday

May 14

16:45 - 17:45

Hall A

Gynaecology

Co-Chair: Elena Manea, Romania;

Chair: , Austria

Session Code: 2510

Session Type: Proffered Papers

Track: Clinical

16:45 - 16:55

Early toxicity and quality of life after molecular-based adjuvant treatment in the PORTEC-4a trial

Anne-Sophie van den Heerik, The Netherlands

Presentation Number: OC-0601

Abstract

Abstract Title:

Early toxicity and quality of life after molecular-based adjuvant treatment in the PORTEC-4a trial

Authors:

Anne-Sophie van den Heerik¹, Cathalijne Post¹, Ludy Lutgens², Dorien Haverkort³, Stefan Kommoss⁴, Friederike Koppe⁵, Marlies Nowee⁶, Henrike Westerveld⁷, Marianne de Jong⁸, David Cibula⁹, Jeltsje Cnossen¹⁰, Jan Willem Mens¹¹, Cyrus Chargari¹², Stefan Bijmolt¹³, Charles Gillham¹⁴, Tanja Stam¹⁵, Ina Jurgenliemk-Schulz¹⁶, Katrien Vandecasteele¹⁷, Karen Verhoeven-Adema¹⁸, Remi Nout^1,11, Hein Putter¹⁹, Vincent Smit²⁰, Nanda Horeweg¹, Tjalling Bosse²⁰, Carien Creutzberg¹

¹Leiden University Medical Center, Radiation Oncology, Leiden, The Netherlands; ²Maastricht Radiation Oncology Clinic, Radiation Oncology, Maastricht, The Netherlands; ³Radiotherapy Group, Radiation Oncology, Arnhem, The Netherlands; ⁴University of Tübingen, Women’s Health, Tübingen, Germany; ⁵Institute Verbeeten, Radiation Oncology, Tilburg, The Netherlands; ⁶Netherlands Cancer Institute, Radiation Oncology, Amsterdam, The Netherlands; ⁷Amsterdam University Medical Centers, Radiation Oncology, Amsterdam, The Netherlands; ⁸Radiotherapy Institute Friesland, Radiation Oncology, Leeuwarden, The Netherlands; ⁹First Faculty of Medicine, Charles University and General University Hospital, Obstetrics and Gynaecology, Prague, Czech Republic; ¹⁰Catharina Hospital, Radiation Oncology, Eindhoven, The Netherlands; ¹¹Erasmus MC – Cancer Institute, Radiation Oncology, Rotterdam, The Netherlands; ¹²Institut Gustave Roussy, Radiation Oncology, Villejuif, France; ¹³University Medical Center Groningen, Radiation Oncology, Groningen, The Netherlands; ¹⁴St. Luke’s Hospital, Radiation Oncology, Dublin, Ireland; ¹⁵Haaglanden Medical Center, Radiation Oncology, The Hague, The Netherlands; ¹⁶University Medical Center Utrecht, Radiation Oncology, Utrecht, The Netherlands; ¹⁷University Hospital Ghent, Radiation Oncology, Ghent, Belgium; ¹⁸Comprehensive Cancer Centre Utrecht, IKNL, Utrecht, The Netherlands; ¹⁹Leiden University Medical Center, Medical Statistics, Leiden, The Netherlands; ²⁰Leiden University Medical Center, Pathology, Leiden, The Netherlands

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Purpose or Objective

The international PORTEC-4a trial was the first trial to incorporate molecular factors in decision making on adjuvant treatment for women with early stage high-intermediate risk endometrial cancer (HIR-EC). For patients allocated to the intervention arm, adjuvant treatment was based upon a molecular-integrated risk profile. The present analyses were performed to compare health-related quality of life (HRQL) and adverse event (AE) rates between the treatment arms in the first 6 months after randomisation.

Material and Methods

Patients with HIR-EC were randomised (2:1) between individualised treatment based upon a molecular-integrated risk profile or standard vaginal brachytherapy (VBT). In case of a favourable profile, adjuvant treatment was omitted. Those with an intermediate profile received VBT while those with an unfavourable risk profile received pelvic radiotherapy (EBRT). HRQL was assessed with the EORTC-QLQ C30 and EN24 module at baseline, after treatment and 6 monthly after randomisation. AE were graded using the CTCAE v4.0. Analyses were performed on the per-protocol population. Prevalence of toxicity was calculated at each timepoint and compared using Fisher’s exact test. Analysis of HRQL was done according to the EORTC guidelines. Symptoms rated as “quite a bit” or “very much” were considered ‘severe’. A 2-sided p<0.01 was considered statistically significant, and p<0.05 reported as a trend.

Results

Between 2012 and 2021, 563 evaluable patients were included, 367 in the molecular arm vs 196 in the standard arm, see figure 1. In 46.7% of patients in the molecular arm adjuvant treatment was omitted. Grade ≥2 AE were reported in 59 patients at completion of treatment: 41 (11.4%) in the interventional arm vs 18 (8.9%) in the standard arm (p=0.39); at 6 months, this was 44 (12.2%) vs 22 (10.9%), p=0.36. Grade 3 AE were reported for 4 patients (3 in the molecular arm and 1 in the standard arm) at treatment completion, and for 8 (4 vs 4) at 6 months. There were no grade 4 or 5 AE. During treatment all grade 3 AE were genitourinary or vaginal, whereas at 6 months only 1 was related to treatment. 94.7% completed HRQL assessment at baseline, 81.0% during treatment and 82.2% at 6 months. No significant differences between the two arms were found for physical functioning (p=0.31) and global health status (p=0.10). Social and role functioning improved over time in both arms (p<0.001). A trend for better role functioning over time was seen for patients treated according to their molecular profile compared to standard VBT (p=0.014).

Conclusion

Use of adjuvant treatment was greatly reduced by individualised treatment in the molecular arm of the PORTEC-4a trial. In the first 6 months no significant difference in early toxicity and HRQL were found between molecular-based adjuvant treatment and standard brachytherapy, while a strong trend for better role functioning after individualised treatment was observed.