What question did this study set out to answer?

This research aims to identify relapse patterns and treatment effectiveness after first-line platinum chemotherapy in advanced epithelial ovarian cancer.

May 30, 2026

Progression patterns and management after frontline platinum in advanced epithelial ovarian cancer (EOC).

Key Points

This research aims to identify relapse patterns and treatment effectiveness after first-line platinum chemotherapy in advanced epithelial ovarian cancer.
Retrospective analysis of 107 advanced EOC patients treated with platinum-based chemotherapy and/or surgery.
Progression categorized into oligoprogression (1-5 lesions) or multiple progression.
Survival outcomes estimated using Kaplan-Meier and compared via Cox regression.
Among 75 relapsed patients, 39% had oligoprogression with longer median overall survival of 110.4 months.
Oligoprogressive group had higher rates of frontline PARP inhibitor maintenance (93% vs 31%; p=0.02).
Local therapy significantly improved overall survival (102.6 months vs 34.3 months; p<0.001).

Abstract

e17581 Background: Most patients with EOC relapse after frontline platinum-based chemotherapy, even with maintenance therapy. Oligoprogression may define a distinct, locally treatable relapse pattern. Methods: We retrospectively analyzed advanced EOC patients treated at our institution (January/2014–December/2024) with surgery and platinum-based chemotherapy, or achieving radiologic complete response after frontline platinum chemotherapy without surgery. Progression was categorized as oligoprogression (1–5 lesions; group A) or multiple progression (group B). Associations were assessed using chi-square tests. Survival outcomes were estimated by Kaplan–Meier and compared by Cox regression. Baseline characteristics are summarized in the Table. Results: Among 107 patients (mean age 65±9.3 years), 75 (70%) relapsed and 29/75 (39%) had oligoprogression. Group A had a higher rate of frontline PARP inhibitor (PARPi) maintenance than group B (14/15 vs 11/35; p=0.02) and fewer metastatic sites at relapse (p=0.01). In the overall cohort, progression-free survival (PFS) >12 months from the end of frontline chemotherapy was associated with a higher likelihood of receiving local vs systemic therapy (p=0.002). In group A, median overall survival (OS) was 110.4±32.4 months and median PFS was 12.5±0.88 months. Local therapy (surgery and/or radiotherapy) versus systemic therapy was associated with longer OS (102.6 vs 34.3 months; p12 months showed a trend toward longer PFS (25.4 vs 13.4 months; p=0.053). Excluding bevacizumab, PARPi >12 months versus ≤12/no maintenance showed a non-significant trend toward longer PFS (24.5 vs 13.1 months; p=0.10). Conclusions: In this real-world cohort, frontline PARPi maintenance was associated with a higher proportion of oligoprogressive relapse. Among oligoprogressive patients, local therapy was associated with clinically meaningful OS and PFS prolongation, supporting its consideration within multidisciplinary post-progression management. Characteristic Group A (n=29) (%) Group B (n=46) (%) Stage III / IV 51.7 / 48.3 69.6 / 30.4 Debulking surgery(S)/ Interval S/ no S 37.9 / 58.6 / 3.4 43.5/ 54.3 / 2.2 Chemotherapy (CT): neoadjuvant / adjuvant / palliative 58.6 / 31 / 10.3 50 / 39.1 / 10.9 HRD status: HRD+/ BRCA +, HRD+/ BRCA -, HRP, unknown 10.3 / 0 / 10.3 / 79.3 4.3 / 0 / 10.9 / 84.8 Germline BRCA status: BRCA1 / BRCA2 / wild-type / unknown 6.9 / 13.8 / 55.2 / 24.1 8.7 / 2.2 / 71.7 / 17.4 Maintenance therapy: bevacizumab / PARPi/ no maintenance 13.8 / 48.3/ 37.9 16.7 / 23.9/ 59.4 Relapse metastatic sites: 1 / 2 / 3 / 4 / 5 86.2 / 13.8 / 0 / 0 / 0 54.3 / 32.6 / 13 / 0 / 0 Progression sites (non-mutually exclusive): peritoneal/lymph nodes/liver/pleura/other 62.1 / 24.1 / 10.3 / 3.4 / 20.6 82.6 / 41.3 / 15.2 / 15.2 / 6.5 Treatment at relapse: S/radiotherapy/CT/S and CT/no therapy 31 / 6.9 / 34.5 / 24.1 / 3.4 0 / 0 / 93.5 / 4.3 / 2.2

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