The use of olaparib as a monotherapy or in combination with cediranib did not provide a statistically significance overall survival (OS) benefit compared with standard of care platinum-based chemotherapy in patients with recurrent, platinum-sensitive ovarian cancer.
This article was originally published by OncLive®. This version has been lightly edited.
The use of olaparib (Lynparza) as a monotherapy or in combination with cediranib did not provide a statistically significance overall survival (OS) benefit compared with standard of care platinum-based chemotherapy in patients with recurrent, platinum-sensitive ovarian cancer, according to the final report of survival outcomes from the randomized phase 3 NRG-GY004 trial.
These findings were published as a supplement in Annals of Oncology and presented during the 2023 ESMO Congress.1 They showed that chemotherapy among 187 patients resulted in a median OS of 32.7 months compared with 33.5 months for olaparib plus cediranib among 189 patients (HR, 1.12; 95% CI, 0.874-1.43; P = .0378) and 31.0 months for olaparib alone among another 189 patients (HR, 1.27; 95% CI, 0.990-1.62; P = .060).
Further assessment of OS outcomes based on BRCA mutational status showed that patients with a germline BRCA1/2 mutation experienced a numerically higher median OS across all 3 treatment arms. The median OS was 43.2 months, 44.8 months, and 41.3 months in the chemotherapy (n = 44), olaparib/cediranib (n = 45; HR, 1.26; 95% CI, 0.71-2.21), and olaparib monotherapy (n = 45; HR, 1.39; 95% CI, 0.80-2.42) arms, respectively. Conversely, patients without these mutations experienced a median OS of 30.0 months, 29.6 months, and 24.5 months with the chemotherapy (n = 143), olaparib combination therapy (n = 144; HR, 1.07; 95% CI, 0.82-1.40), and olaparib monotherapy (n = 144; HR, 1.24; 95% CI, 0.94-1.63) regimens, respectively.
“When we look at OS, neither olaparib nor the combination of cediranib and olaparib improved OS compared with chemotherapy regardless of germline BRCA status,” Joyce F. Liu, MD, MPH, lead study author, stated in an oral presentation of the data. Liu is an associate chief of the Division of Gynecologic Oncology, director of Clinical Research in the Division of Gynecologic Oncology, associate clinical research officer of the Clinical Research Program, and a physician at Dana-Farber Cancer Institute, as well as associate professor of medicine at Harvard Medical School.
This randomized, open-label, study enrolled patients with measurable or evaluable platinum-sensitive relapsed high-grade serous or high-grade endometrioid ovarian cancer, primary peritoneal cancer, or fallopian tube cancer. Eligible patients were also required to have been treated with up to 1 prior platinum-based chemotherapy and experienced disease recurrence no less than 6 months after their most recent chemotherapy treatment. Key exclusion criteria included prior treatment with a PARP inhibitor or antiangiogenic therapy in the recurrent setting, with the exception of bevacizumab.
Patients were stratified by germline BRCA status, prior platinum-free intervals (PFI), and whether they had received prior antiangiogenic therapy. They were randomly assigned 1:1:1 to receive 300 mg of olaparib twice a day, 200 mg of olaparib twice daily and 30 mg of cediranib once daily, or 1 of 3 platinum-doublet chemotherapy regimens per investigator’s choice. Chemotherapy regimens could include carboplatin plus paclitaxel, carboplatin plus gemcitabine, or carboplatin plus liposomal doxorubicin. The olaparib regimens were continuously dosed.
Patients assigned to the chemotherapy arm could continue treatment for as long as medically appropriate. All patients who completed chemotherapy did not receive further therapy and were followed until disease progression, while patients in either olaparib arm continued treatment until disease progression, intolerable toxicity, or withdrawal. Radiographic tumor assessments were done every 9 weeks for 12 months, followed by every 12 weeks until disease progression.
The study’s primary end point was progression-free survival (PFS), and key secondary end points included OS, tumor objective response rate, and the agent’s clinical activity in biomarker-defined populations.
Previously reported data from NRG-GY004 showed that neither cediranib plus olaparib nor olaparib alone met the primary end point of improved PFS compared with platinum-based chemotherapy (HR, 0.86; 95% CI, 0.66-1.10; P = .077). However, the regimens did produce similar antitumor activity. The median PFS in the intention-to-treat population was 10.3 months (95% CI, 8.7-11.2), 10.4 months (95% CI, 8.5-12.5), and 8.2 months (95% CI, 6.6-8.7) with chemotherapy, the olaparib combination, and olaparib monotherapy, respectively. Corresponding overall response rates were 71.3% (95% CI, 63.4-78.1), 69.4% (95% CI, 61.8-76.1), and 52.4% (95% CI, 44.8-60.1). Clinical activity seen with the olaparib regimens was particularly notable in patients harboring germline BRCA mutations.2
Based on these data, investigators assessed the effect of these all-oral, non-platinum regimens on OS in this population, which was a preplanned, non-analytical end point.
It's important to note that the majority of patients across the 3 chemotherapy, comination therapy, and monotherapy arms had the following characteristics:
Additionally, most patients had received 1 prior line of therapy (66.8%; 64.6%; 64.6%) followed by 2 prior lines (24.6%; 28.6%; 28.0%), then 3 or more lines (8.6%; 6.9%; 7.4%).
Germline BRCA mutations were observed in 23.5%, 23.8%, and 23.8% of patients in the chemotherapy, combination therapy, and monotherapy arms, respectively. The percentage of patients with a PFI of over 12 months was 49.2%, 50.3%, and 49.7%, and the corresponding percentages for patients with a PFI of 6 to 12 months were 50.8%, 47.9%, and 50.3%, respectively.
The final OS analysis was conducted upon the occurrence of at least 265 deaths among participants assigned to either the chemotherapy arm or the combination arm. The study aimed for approximately 80% power, assuming proportional hazards, to detect a 30% reduction in the hazard of death (HR, 0.70), with a type I error set to 0.025 for a one-tailed test. Since the PFS end point was not met, a formal interpretation of OS analyses was not conducted. Data collection ended on March 7, 2023, after 266 events were reported in these 2 treatment arms.
Among all enrolled patients, a total of 419 deaths were reported, with 60 patients still alive by the time of data analysis. In the chemotherapy arm, 27.3% of patients withdrew from the study, including 6 patients who withdrew after disease progression. Withdrawals also occurred in 7.9% of patients in the combination arm and 10.6% of those in the monotherapy arm, with 7 and 5 withdrawals occurring after progression in these respective arms.
Data from the updated analysis of PFS according to BRCA mutational status showed that patients with BRCA1/2 mutations experienced a median OS of 10.5 months with chemotherapy, 18.0 months with olaparib plus cediranib (HR, 0.56; 95% CI, 0.33-0.95), and 12.7 months with olaparib monotherapy (HR, 0.65; 95% CI, 0.39-1.09). In the BRCA1/2 wild-type population, the median PFS was 9.7 months, 8.9 months, and 6.6 months, and 8.9 months for the chemotherapy, combination (HR, 0.98; 95% CI, 0.74-1.30), and monotherapy (HR, 1.39; 95% CI, 1.05-1.84) arms, respectively.
The overall incidence of therapy-related myelodysplastic syndrome (MDS) and acute myeloid leukemia (AML) in the study was low. A total of 5 events were observed, including 3 MDS events and 2 AML events, and both AML events occurred in patients treated with cediranib plus olaparib. Meanwhile, 2 MDS events occurred with the olaparib combination, and 1 event occurred with carboplatin plus paclitaxel. Notably, 1 patient harboring a BRCA mutation had an MDS event while being treated with cediranib plus olaparib. The remaining 4 patients did not experience an MDS or AML event on study treatment.
Investigators noted that caution should be exhibited when interpreting results, as a high proportion of patients withdrew early from survival follow-up, particularly in the control arm.
“These results are also confounded by the number of patients who crossed over to receive a PARP inhibitor at some point on the SOC arm…we are looking at the additional crossover events,” Liu concluded.
References
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