Methods | Open‐label, randomised, phase II, multicentre study Randomisation (1:1) stratified by number of platinum treatments and platinum‐free interval |
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Participants | 162 women with platinum‐sensitive recurrent high‐grade serous epithelial ovarian cancer Baseline characteristics well balanced between groups. However, 6 randomised to placebo arm withdrew before starting treatment compared to 0 in the OLA group Median age 59.0 (range 27 to 78) (Arm A) 62 (Arm B) (range 31 to 79) |
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Interventions |
Arm A ‐ OLA orally (200 mg bd days 1 to 10 of a 21‐day cycle) in combination with paclitaxel (P) intravenous (IV) (175 mg/m2 day 1 of a 21‐day cycle) and carboplatin (C) IV (AUC4 day 1 of a 21‐day cycle) for at least 4 cycles. Followed by OLA monotherapy maintenance (400 mg bd continuous dosing) Arm B ‐ Paclitaxel (P) IV (175 mg/m2 day 1 of a 21‐day cycle) and carboplatin (C) IV (AUC6 day 1 of a 21‐day cycle) for 6 cycles. Followed by a post‐completion phase in which no study treatment was administered |
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Outcomes | Primary outcome: progression‐free survival (PFS) by central review (RECIST 1.1) Secondary outcomes: overall survival (OS); objective response rate (ORR); safety 162 women randomised (n = 81 per arm): 156 received treatment (Arm A, n = 81; Arm B, n = 75) and 121 began the maintenance/no further therapy phase (Arm A, n = 66; Arm B, n = 55) Survival and response outcomes OLA + P/C (AUC4) followed by maintenance OLA showed improvement in PFS versus P/C (AUC6) alone (HR 0.51, 95% CI 0.34 to 0.77; P value = 0.0012; median PFS = 12.2 months (95% CI 9.7 to 15.0) versus 9.6 months (95% CI 9.1 to 9.7) OS data (HR 1.17, 95% CI 0.79 to 1.73; P value = 0.4379; median 33.8 versus 37.6 months; 54/81 versus 47/81 deaths in arms A and B respectively; total events = 62%) ORR was similar for Arm A and Arm B (64% versus 58%) Toxicity data (during chemo +/‐ OLA phase) Nausea (G3 to 4): 1/81 (1.2%) (Arm A) and 1/75 (1.3%) (Arm B) Fatigue (G3 to 4): 6/81 (7.4%) (arm A versus 3/75 (4.0%) (Arm B) Abdominal pain: Grade 3 to 4: 0/81 (0%) versus 2/75 (2.67%) (Arm B) Vomiting: Grade 3 to 4: 1/81 (1.23%) versus 0/75 (0%) (Arm B) Anaemia: Grade 3 to 4: 7/82 (8.6%) versus 5/75 (6.7%) Neutropenia: Grade 3 to 4: 35/81 (43.2%) (Arm A) versus 26/75 (34.7%) (Arm B) Toxicity data (during maintenance phase) Nausea (G3 to 4): 1/66 (1.2%) (Arm A) and 0/55 (0%) (Arm B) Fatigue (G3 to 4): 0/66 (0%) (arm A versus 0/55 (0%) (Arm B) Abdominal pain: Grade 3 to 4: 0/66 (0%) versus 0/55 (0%) (Arm B) Vomiting: Grade 3 to 4: 0/66 (1.23%) versus 0/55 (0%) (Arm B) Anaemia: Grade 3 to 4: 5/66 (7.6%) versus 1/55 (1.8%) Neutropenia: Grade 3 to 4: 3/66 (4.5%) (Arm A) versus 0/55 (0%) (Arm B) |
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Notes | We contacted authors for additional information and they provided us with the in‐press manuscript | |
Risk of bias | ||
Bias | Authors' judgement | Support for judgement |
Random sequence generation (selection bias) | Low risk | "Patient randomisation was stratified (using an interactive voice response [IVR]system) based on:1) number of prior platinum‐containing treatment lines received(1 or >1) and 2) time to disease progression following completion of the previous platinum‐containing therapy(>6 to <=12 months or >12 months)." |
Allocation concealment (selection bias) | Low risk | See above |
Blinding of participants and personnel (performance bias) All outcomes | High risk | Open‐label |
Blinding of outcome assessment (detection bias) All outcomes | Low risk | Assessors for central RECIST review were blinded to treatment groups |
Incomplete outcome data (attrition bias) All outcomes | Unclear risk | All patients accounted for from randomisation, although 6 patients in control group withdrew before starting treatment |
Selective reporting (reporting bias) | Low risk | Outcomes pre‐specified on clinical trial registry website |
Other bias | Unclear risk | Industry‐sponsored by AstraZeneca with several authors disclosing financial conflict of interest |
bd: twice a day CI: confidence interval CT: computerised tomography GCIG: Gynaecologic Cancer Intergroup HR: hazard ratio IV: intravenous OLA: olaparib OR: odds ratio ORR: objective response rate OS: overall survival PFS: progression‐free survival PLD: pegylated liposomal doxorubicin PS: performance status pts: patients RECIST: Response Evaluation Criteria in Solid Tumours