Medical Oncology Department, Vall d'Hebron University Hospital and Breast Cancer Group, Vall d'Hebron Institute of Oncology, Barcelona, Spain.
Medical Center Verum, Kyiv, Ukraine.
Lancet Oncol. 2024 Nov;25(11):1424-1439. doi: 10.1016/S1470-2045(24)00387-5.
Resistance to endocrine therapies in hormone receptor-positive breast cancer is challenging. We aimed to assess the next-generation oral selective oestrogen receptor degrader (SERD) and complete oestrogen receptor antagonist, camizestrant, versus the first-approved SERD, fulvestrant, in post-menopausal women with oestrogen receptor-positive, HER2-negative, advanced breast cancer.
SERENA-2 is an open-label, randomised, phase 2 trial that is being conducted at 74 study centres across Asia, Europe, the Middle East, and North America. Female patients aged 18 years or older who were post-menopausal with histologically or cytologically confirmed metastastic or locoregional oestrogen receptor-positive, HER2-negative breast cancer, an Eastern Cooperative Oncology Group or WHO performance status of 0 or 1, and disease recurrence or progression on at least one line of endocrine therapy, and no more than one previous endocrine therapy in the advanced setting. Patients were initially randomly assigned (1:1:1:1) to receive oral camizestrant once daily at 75 mg, 150 mg, or 300 mg (until the 300 mg group was closed), or fulvestrant intramuscularly at 500 mg (per label). Randomisation was managed through an interactive web-based system and stratified by previous treatment with CDK4/6 inhibitors and presence of liver and/or lung metastases. The primary objective was to determine clinical efficacy of camizestrant versus fulvestrant at each dose level using the primary endpoint of investigator-assessed progression-free survival, per Response Evaluation Criteria in Solid Tumours (version 1.1), assessed by intention to treat in all randomly assigned patients (full analysis set). No formal statistical comparison for the efficacy analysis of the camizestrant 300 mg dose versus fulvestrant was to be performed. Safety analyses included all randomly assigned patients who received at least one dose of study treatment. This study is registered with ClinicalTrials.gov, NCT04214288, and is ongoing.
Between May 11, 2020, and Aug 10, 2021, 240 patients were randomly assigned to receive camizestrant 75 mg (n=74), 150 mg (n=73), 300 mg (n=20), or fulvestrant (n=73), and were included in the full analysis set. All patients received at least one dose of study drug. Median follow-up was 16·6 months (IQR 12·9-19·4) for the camizestrant 75 mg group, 16·3 months (12·9-18·3) for the camizestrant 150 mg group, and 14·7 months (12·7-20·1) for the fulvestrant 500 mg group. Median progression-free survival was 7·2 months (90% CI 3·7-10·9) with camizestrant 75 mg, 7·7 months (5·5-12·9) with camizestrant 150 mg, and 3·7 months (2·0-6·0) with fulvestrant. The hazard ratio for camizestrant 75 mg versus fulvestrant was 0·59 (90% CI 0·42-0·82; p=0·017), and the hazard ratio for camizestrant 150 mg versus fulvestrant was 0·64 (0·46-0·89; p=0·0090). Treatment-related adverse events occurred in 39 (53%) of 74 patients in the camizestrant 75 mg group, 49 (67%) of 73 patients in the camizestrant 150 mg group, 14 (70%) of 20 patients in the camizestrant 300 mg group, and 13 (18%) of 73 patients in the fulvestrant group. No single grade 3 or worse treatment-emergent adverse event occurred in more than two (3%) patients in any group. Serious treatment-emergent adverse events occurred in six (8%) patients in the camizestrant 75 mg group, seven (10%) patients in the camizestrant 150 mg group, two (10%) patients in the camizestrant 300 mg group, and four (5%) patients in the fulvestrant group. No treatment-related deaths occurred.
Camizestrant at 75 and 150 mg showed a significant benefit in progression-free survival versus fulvestrant. These results support further development of camizestrant for the treatment of oestrogen receptor-positive, HER2-negative breast cancer.
AstraZeneca.
激素受体阳性乳腺癌对内分泌治疗的耐药性是一个挑战。我们旨在评估下一代口服选择性雌激素受体降解剂(SERD)和完全雌激素受体拮抗剂卡米昔司他与第一代批准的 SERD 氟维司群在绝经后雌激素受体阳性、HER2 阴性、晚期乳腺癌女性中的疗效。
SERENA-2 是一项正在亚洲、欧洲、中东和北美 74 个研究中心进行的开放标签、随机、2 期试验。入组患者为年龄 18 岁或以上的绝经后女性,组织学或细胞学证实转移性或局部复发性雌激素受体阳性、HER2 阴性乳腺癌,东部合作肿瘤学组或世界卫生组织体能状态为 0 或 1,并且在至少一线内分泌治疗后疾病复发或进展,在晚期治疗中,之前接受的内分泌治疗不超过 1 次。患者最初按 1:1:1:1 的比例随机分配(1:1:1:1)接受每日一次 75mg、150mg 或 300mg 卡米昔司他(直至 300mg 组关闭)或 500mg 氟维司群肌内注射(按说明书)。随机分组通过交互式网络系统进行管理,并按之前使用 CDK4/6 抑制剂和存在肝转移和/或肺转移分层。主要终点是通过在意向治疗的所有随机分配患者(全分析集)中使用研究者评估的无进展生存期作为主要疗效终点,评估卡米昔司他与氟维司群在每个剂量水平的临床疗效。不进行卡米昔司他 300mg 剂量与氟维司群的疗效分析的正式统计学比较。安全性分析包括所有接受至少一剂研究治疗的随机分配患者。该研究在 ClinicalTrials.gov 注册,编号为 NCT04214288,正在进行中。
2020 年 5 月 11 日至 2021 年 8 月 10 日,240 名患者被随机分配接受卡米昔司他 75mg(n=74)、150mg(n=73)、300mg(n=20)或氟维司群(n=73),并纳入全分析集。所有患者均接受了至少一剂研究药物。卡米昔司他 75mg 组的中位随访时间为 16.6 个月(IQR 12.9-19.4),卡米昔司他 150mg 组为 16.3 个月(12.9-18.3),氟维司群 500mg 组为 14.7 个月(12.7-20.1)。卡米昔司他 75mg 组的中位无进展生存期为 7.2 个月(90%CI 3.7-10.9),卡米昔司他 150mg 组为 7.7 个月(5.5-12.9),氟维司群组为 3.7 个月(2.0-6.0)。卡米昔司他 75mg 与氟维司群的风险比为 0.59(90%CI 0.42-0.82;p=0.017),卡米昔司他 150mg 与氟维司群的风险比为 0.64(90%CI 0.46-0.89;p=0.0090)。卡米昔司他 75mg 组有 39 名(53%)患者和氟维司群组有 13 名(18%)患者发生与治疗相关的不良事件(p=0.017)。卡米昔司他 75mg 组、卡米昔司他 150mg 组、卡米昔司他 300mg 组和氟维司群组分别有 39(53%)、49(67%)、14(70%)和 13(18%)例患者发生 3 级或以上治疗相关不良事件。任何一组均无 2 例(3%)以上患者发生任何 1 例 3 级或更严重的治疗相关不良事件。卡米昔司他 75mg 组有 6 名(8%)患者、卡米昔司他 150mg 组有 7 名(10%)患者、卡米昔司他 300mg 组有 2 名(10%)患者和氟维司群组有 4 名(5%)患者发生严重治疗相关不良事件。无治疗相关死亡。
卡米昔司他 75mg 和 150mg 与氟维司群相比,无进展生存期有显著获益。这些结果支持进一步开发卡米昔司他用于治疗雌激素受体阳性、HER2 阴性乳腺癌。
阿斯利康。
