Laurence Gladieff

Pocket memo based on the ESGO/ESTRO/ESP guidelines for the management of patients with endometrial carcinoma: definition of prognostic risk groups

Association between molecular classification and overall survival in patients with metastatic endometrial carcinoma: ancillary results of the UTOLA phase II GINECO trial

We aimed to describe the association between molecular sub-groups and outcomes in patients with advanced/metastatic endometrial carcinoma amenable to maintenance/active surveillance after carboplatin-based chemotherapy. Patients treated in the GINECO trial UTOLA (NCT03745950, randomly allocating patients 2:1 to olaparib/placebo after tumor control under carboplatin-based chemotherapy), with prospective centralized targeted next-generation sequencing, and mismatch repair and p53 immunostainings were included. Next-generation sequencing (667.5 kb) included POLE (exo-nuclease domain), TP53, PIK3CA, PIK3R1, PTEN, KRAS, and CTNNB1. Tumors were categorized following the 2022 European Society of Gynaecological Oncology/European Society for Radiotherapy and Oncology/European Society of Pathology guidelines as POLE-mutated, mismatch repair-deficient, p53-abnormal (immunostaining or TP53 mutation), and with no specific molecular profile. Exploratory analyses categorized non-p53-abnormal tumors based on literature (mismatch repair-deficient: mutational burden; no specificity: PIK3R1/PTEN wild-type tumors, CTNNB1/KRAS-mutated tumors, others). Among 145 patients in the intention to treat population (median follow-up 31 months), 1, 21 (15%), 76 (53%), and 45 (32%) had POLE, mismatch repair-deficient, p53-abnormal, and non-specific tumors (2 missing mismatch repair), respectively. Molecular characterization was associated with progression-free (log-rank, p = .017) and overall survival (p < .001). Patients with p53abn tumors had a hazard ratio for death of 2.43, 95% confidence interval 1.50 to 3.93 (adjusted on age, stage IV, measurable lesions after chemotherapy). Exploratory analyses showed high mutational burden mismatch repair-deficient tumors with prognostic similar to p53abn tumors, whereas tumors with lower mutational burden had better progression-free survival. PIK3R1/PTEN wild-type and CTNNB1/KRAS-mutated non-specific tumors had better outcomes than p53abn tumors. Other non-specific tumors have survival similar to p53abn tumors. Integration of molecular sub-group as a stratification parameter might be considered for randomized trials in advanced/metastatic endometrial carcinoma after carboplatin-based chemotherapy. Deeper characterization of mismatch repair-proficient tumors might enhance prognostication.

Surgical approach and maintenance therapy in advanced low-grade serous ovarian cancer: Insights from the French ESME database

Low-grade serous ovarian cancer is a rare sub-type characterized by indolent growth, limited therapeutic options, and relative chemoresistance. This study aimed to describe management patterns, survival outcomes, and the efficacy of systemic therapies in a large cohort of patients with low-grade serous ovarian carcinoma treated across 18 French comprehensive cancer centers. Using data from the Epidemiological Strategy and Medical Economics ovarian cancer database (NCT03275298), patients with International Federation of Gynecology and Obstetrics (FIGO) stage III to IV low-grade serous ovarian carcinoma diagnosed between 2011 and 2024 were examined. Clinical outcomes, overall survival, and progression-free survival were assessed, along with treatment-related factors affecting survival, including surgical management and bevacizumab administration. Univariable and multi-variable analyses were conducted using Kaplan-Meier estimates and Cox proportional hazards models. Among 230 patients with low-grade serous ovarian carcinoma (median age 55.5 years [range; 19.8-88.2]), 171 (74.3%) and 59 (25.7%) had FIGO stage III and IV diseases, respectively. Primary debulking surgery was performed in 128 (55.6%), platinum-based chemotherapy was given to 223 (97%), and bevacizumab was administered to 79 (34.3%) patients. The median follow-up period was 73.6 months (95% confidence interval [CI] 69.9 to 80.0). Patients who underwent primary debulking surgery had the longest median progression-free survival (35.2 months, 95% CI 26.5 to 48.1) and overall survival (146 months, 95% CI 110.4 to not reached). Multi-variable analyses identified FIGO stage and primary debulking surgery as key prognostic factors for overall survival, whereas age and bevacizumab use were not significantly associated with outcomes. This real-world study underscores the prognostic relevance of surgical approach and disease stage in low-grade serous ovarian carcinoma. Continued investigation is warranted to define the optimal integration of emerging systemic therapies and improve outcomes in this rare malignancy.

Pembrolizumab or Placebo Plus Adjuvant Chemotherapy With or Without Radiotherapy for Newly Diagnosed, High-Risk Endometrial Cancer: Results in Mismatch Repair-Deficient Tumors

Mismatch repair-deficient (dMMR) endometrial cancer (EC) is an inflamed phenotype with poor outcomes when meeting high-risk criteria and limited treatment options in the adjuvant setting. We report protocol-prespecified subgroup analysis of patients with dMMR tumors from the phase III ENGOT-en11/GOG-3053/KEYNOTE-B21 study (ClinicalTrials.gov identifier: NCT04634877 ) in newly diagnosed, high-risk EC after surgery with curative intent. Patients were randomly assigned to pembrolizumab 200 mg or placebo (six cycles) plus carboplatin-paclitaxel (four to six cycles) once every 3 weeks, then pembrolizumab 400 mg or placebo once every 6 weeks (six cycles), respectively. MMR status was a stratification factor. Patients received radiotherapy at investigator discretion. Investigator-assessed disease-free survival (DFS) was a primary end point. No formal hypothesis testing was performed for subgroup analysis. In the intention-to-treat population, 141 patients in the pembrolizumab arm and 140 in the placebo arm had dMMR tumors. At this interim analysis, hazard ratio for DFS favored pembrolizumab (0.31 [95% CI, 0.14 to 0.69]); median DFS was not reached in either group. Two-year DFS rates were 92.4% (95% CI, 84.4 to 96.4) and 80.2% (95% CI, 70.8 to 86.9), respectively. No new safety signals occurred. Longer-term follow-up of outcomes will be evaluated at final analysis. Preplanned subgroup analysis on the basis of the study's stratification factors suggests that pembrolizumab plus chemotherapy improves DFS and is clinically relevant for patients with dMMR tumors in the curative-intent setting.

Clinical Trial Protocol for ROSELLA: a phase 3 study of relacorilant in combination with nab-paclitaxel versus nab-paclitaxel monotherapy in advanced platinum-resistant ovarian cancer

Ovarian cancer has the highest mortality among gynecologic cancers, primarily because it typically is diagnosed at a late stage and because of the development of chemoresistance in recurrent disease. Improving outcomes in women with platinum-resistant ovarian cancer is a substantial unmet need. Activation of the glucocorticoid receptor (GR) by cortisol has been shown to suppress the apoptotic pathways used by cytotoxic agents, limiting their efficacy. Selective GR modulation may be able to counteract cortisol's antiapoptotic effects, enhancing chemotherapy's efficacy. A previous phase 2 study has shown that adding intermittently dosed relacorilant, a selective GR modulator, to nab-paclitaxel improved outcomes, including progression-free survival (PFS) and overall survival (OS), with minimal added toxicity, in women with recurrent platinum-resistant ovarian cancer. The ROSELLA study aims to confirm and expand on these findings in a larger population. ROSELLA is a phase 3, randomized, 2-arm, open-label, global multicenter study in women with recurrent, platinum-resistant, high-grade serous epithelial ovarian, primary peritoneal, or fallopian tube cancer. Eligible participants have received 1 to 3 lines of prior systemic anticancer therapy, including ≥1 prior line of platinum therapy and prior treatment with bevacizumab, with documented progressive disease or intolerance to the most recent therapy. There is no biomarker-based requirement for participant selection. Participants are randomized 1:1 to receive intermittently dosed relacorilant in combination with nab-paclitaxel or nab-paclitaxel monotherapy. The study's primary efficacy endpoint is PFS as assessed by blinded independent central review. Secondary efficacy endpoints include OS, investigator-assessed PFS, objective response rate, best overall response, duration of response, clinical benefit rate at 24 weeks, and cancer antigen 125 response. The study is also evaluating safety and patient-reported outcomes. ClinicalTrials.gov Identifier: NCT05257408; European Union Drug Regulating Authorities Clinical Trials Database Identifier: 2022-000662-18.

ctDNA for Prognostication and Monitoring in Patients with Metastatic Endometrial Carcinoma Treated with Olaparib: Validation in the GINECO-UTOLA Trial

Abstract Purpose: ctDNA may offer a noninvasive means to evaluate tumor response and anticipate disease dynamics before radiologic changes in advanced endometrial carcinoma. Experimental Design: This ancillary analysis included patients from the multicenter, randomized, phase II GINECO-UTerin OLAparib (UTOLA) trial (NCT03745950) evaluating olaparib/placebo as maintenance after first-line platinum-based chemotherapy. Plasma samples were collected at screening after chemotherapy (baseline), 3 months (M3), and progression. ctDNA detection was assessed by a validated methylation-based Droplet Digital PCR (MethddPCR) assay targeting DNA positions universally methylated in endometrial carcinoma. Results: Among 130 evaluable patients, ctDNA was detected in 25 of 129 (19%, 1 technical fail) at baseline, 15 of 80 (19%) at M3, and 33 of 52 (63%) at progression. Baseline ctDNA positivity was independently associated with poorer progression-free survival (PFS) [median 1.81 vs. 7.39 months; adjusted HR = 5.33 (3.17–8.97)] and overall survival (OS) [10.3 vs. 24.7 months; adjusted HR = 3.98 (2.28–6.91); adjusted for age, stage IV at diagnosis, p53abn subgroup, and residual measurable lesions after chemotherapy]. Patients with baseline ctDNA had median OS of 9.36 months under olaparib versus 19.6 months under placebo (log-rank P = 0.05). Patients with increasing ctDNA at M3 had median PFS of 1.67 months, versus 9.64 months without, and median OS of 18.8 versus 25.8 months. ctDNA rising was predictive of poor postprogression OS under olaparib but not under placebo (interaction test, P &amp;lt; 0.001). Conclusions: MethddPCR-ctDNA is an independent prognostic biomarker for OS in advanced/metastatic endometrial carcinoma. MethddPCR-ctDNA may identify patients unlikely to benefit from PARP inhibition, guide therapeutic decisions, and should be further evaluated as a new stratification parameter in future endometrial carcinoma trials.