Van Gorp Toon, Moore Kathleen N, Konecny Gottfried E, Leary Alexandra, García-García Yolanda, Banerjee Susana, Lorusso Domenica, Lee Jung-Yun, Moroney John W, Caruso Giuseppe, Klasa-Mazurkiewicz Dagmara, Tromp Jacqueline, Martin Lainie P, Breuer Shani, Leath Charles A, Cibula David, Weroha S John, Estévez-García Purificación, O'Malley David M, Miller Rowan E, Coffman Lan, Scandurra Giuseppa, Berton Dominique, Li Lingling, Zagadailov Erin, Diver Elisabeth J, Trédan Olivier, Hilpert Felix
Leuven Cancer Institute, University Hospitals Leuven and KU Leuven, Leuven, Belgium; Belgium and Luxembourg Gynaecological Oncology Group (BGOG), Leuven, Belgium.
Department of Gynecologic Oncology, OU Health Stephenson Cancer Center, Oklahoma City, OK, USA; Gynecologic Oncology Group Partners (GOG-P), Philadelphia, PA, USA.
Lancet Oncol. 2025 Apr;26(4):503-515. doi: 10.1016/S1470-2045(25)00021-X.
Mirvetuximab soravtansine-gynx (MIRV) is a first-in-class antibody-drug conjugate targeting folate receptor α (FRα), approved by the US Food and Drug Administration for the treatment of platinum-resistant ovarian cancer in the USA. Here, we report patient-reported outcomes for participants treated with MIRV compared with investigator's choice of chemotherapy from the phase 3 MIRASOL trial, which met its primary endpoint of progression-free survival and key secondary endpoints of objective response rate and overall survival.
The MIRASOL trial was a confirmatory, phase 3, randomised, controlled, open-label trial, building on the phase 2 SORAYA trial which had previously demonstrated the safety and efficacy of MIRV in platinum-resistant ovarian cancer. Patients 18 years or older with a confirmed platinum-resistant, recurrent high-grade serous epithelial ovarian cancer diagnosis were recruited from 253 sites including hospitals, academic centres, and community centres in 21 countries. Patients must have received one to three previous systemic anticancer therapies, and have high FRα tumour expression (≥75% tumour cells with an immunohistochemistry score of ≥2+ membrane staining using the PS2+ scoring method), one or more lesions with measurable disease, and an Eastern Cooperative Oncology Group performance status of 0 or 1. Patients were randomly assigned (1:1) to MIRV or investigator's choice of chemotherapy, stratified by number of previous therapy lines and the type of investigator's choice of chemotherapy. Therapies were administered in an open-label manner; MIRV was administered intravenously at 6 mg/kg of adjusted ideal bodyweight every 3 weeks. The primary endpoint was progression-free survival. Key secondary endpoints were objective response rate, overall survival, and a 15·0-point or greater improvement at week 8 or 9 in abdominal and gastrointestinal symptoms using the European Organisation for Research and Treatment of Cancer Quality of Life Questionnaire-Ovarian Cancer Module (EORTC QLQ-OV28) in the intention-to-treat population. The MIRASOL trial was registered at ClinicalTrials.gov (NCT04209855), the Gynecologic Oncology Group (GOG 3045), and the European Network of Gynaecological Oncological Trial Groups (ENGOT-ov55), and is complete.
Between Feb 3, 2020, and Aug 3, 2022, 453 patients were enrolled and randomly assigned to treatment (227 to the MIRV group and 226 to the investigator's choice of chemotherapy group). All patients were female; 301 (66%) participants were White, 53 (12%) were Asian, 13 (3%) were Black, and 86 (19%) were of another race or not reported; 27 (6%) were Hispanic or Latino. The median follow-up for the study, determined by the reverse Kaplan-Meier method, was 13·1 months (95% CI 12·1-14). QLQ-OV28 completion rates were 86% (365 of 425) at baseline and 81% (282 of 349) at week 8 or 9. 34 (21·0%; 95% CI 15·0-28·1) of 162 patients treated with MIRV reported improvement in QLQ-OV28 abdominal and gastrointestinal scores, compared with 23 (15·3%; 10·0-22·1) of 150 patients treated with the investigator's choice of chemotherapy. These differences were not statistically significant (odds ratio 1·5 [95% CI 0·8-2·6]; p=0·26).
MIRV did not seem to impair or improve patient quality of life compared with investigator's choice of chemotherapy. The similar quality-of-life outcomes in the two treatment groups, combined with the previously reported higher efficacy of MIRV compared with single-agent chemotherapy, support MIRV as new treatment option for FRα-positive platinum-resistant ovarian cancer.
AbbVie.
Mirvetuximab soravtansine-gynx(MIRV)是首个靶向叶酸受体α(FRα)的抗体药物偶联物,已获美国食品药品监督管理局批准,用于在美国治疗铂耐药卵巢癌。在此,我们报告了3期MIRASOL试验中接受MIRV治疗的参与者与研究者选择的化疗方案相比的患者报告结局,该试验达到了无进展生存期的主要终点以及客观缓解率和总生存期的关键次要终点。
MIRASOL试验是一项验证性3期随机对照开放标签试验,基于2期SORAYA试验开展,该试验先前已证明MIRV在铂耐药卵巢癌中的安全性和有效性。年龄在18岁及以上、确诊为铂耐药复发性高级别浆液性上皮性卵巢癌的患者,从21个国家的253个地点招募,包括医院、学术中心和社区中心。患者必须先前接受过1至3次全身抗癌治疗,且FRα肿瘤高表达(使用PS2+评分法,免疫组化评分≥2+膜染色的肿瘤细胞≥75%),有一个或多个可测量疾病的病灶,东部肿瘤协作组体能状态为0或1。患者按1:1随机分配至MIRV或研究者选择的化疗方案,按先前治疗线数和研究者选择的化疗方案类型进行分层。治疗以开放标签方式给药;MIRV以每3周6mg/kg调整后的理想体重静脉注射。主要终点是无进展生存期。关键次要终点是客观缓解率、总生存期,以及在意向性治疗人群中,使用欧洲癌症研究与治疗组织生活质量问卷-卵巢癌模块(EORTC QLQ-OV28),在第8周或第9周腹部和胃肠道症状改善15.0分或更多。MIRASOL试验已在ClinicalTrials.gov(NCT04209855)、妇科肿瘤学组(GOG 3045)和欧洲妇科肿瘤试验组网络(ENGOT-ov55)注册,且已完成。
2020年2月3日至2022年8月3日期间,453例患者入组并随机分配接受治疗(227例至MIRV组,226例至研究者选择的化疗组)。所有患者均为女性;301例(66%)参与者为白人,53例(12%)为亚洲人,13例(3%)为黑人,86例(19%)为其他种族或未报告;27例(6%)为西班牙裔或拉丁裔。通过反向Kaplan-Meier方法确定该研究的中位随访时间为13.1个月(95%CI 12.1-14)。QLQ-OV28完成率在基线时为86%(425例中的365例),在第8周或第9周时为81%(349例中的282例)。162例接受MIRV治疗的患者中有34例(21.0%;95%CI 15.0-28.1)报告QLQ-OV28腹部和胃肠道评分有所改善,而150例接受研究者选择的化疗方案治疗的患者中有23例(15.3%;10.0-22.1)报告有所改善。这些差异无统计学意义(比值比1.5[95%CI 0.8-2.6];p=0.26)。
与研究者选择的化疗方案相比,MIRV似乎并未损害或改善患者生活质量。两个治疗组相似的生活质量结果,加上先前报告MIRV与单药化疗相比具有更高疗效,支持MIRV作为FRα阳性铂耐药卵巢癌的新治疗选择。
艾伯维公司。
