Beex L, Rose C, Mouridsen H, Jassem J, Nooij M, Estape J, Paridaens R, Piccart M, Gorlia T, Lardenoije S, Baila L
Department of Medical Oncology, 452 Radboud University Nijmegen Medical Centre, P.O. Box 9101, 6500 HB Nijmegen, The Netherlands, and Department of Oncology, Lund University Hospital, Sweden.
Eur J Cancer. 2006 Dec;42(18):3178-85. doi: 10.1016/j.ejca.2006.08.020. Epub 2006 Oct 12.
Continuous ligand depletion of endocrine responsive tumours may enhance resistance to therapy. Intermittent treatment with tamoxifen (T) was considered to mimic (incomplete) ligand depletion and reintroduction. Furthermore it was postulated that alternating tamoxifen with a non-cross resistant endocrine modality could (further) postpone hormone resistance.
Postmenopausal patients with advanced breast cancer who did not progress after 4 months of first line T therapy were randomised to continue T (40 mg daily) or to 2 monthly intermittent T or intermittent/alternated T and medroxyprogesterone acetate (MPA, 300 mg daily). At progression during break or during MPA, T should be reintroduced. Endpoints of the study were progression free survival (PFS), time to resistance to tamoxifen and overall survival (OS).
Of 593 registered patients, 276 were randomised. After 8 years follow-up the median PFS for continuous T, intermittent T and intermittent/alternated T and MPA was 11.0 (8.1-15.2), 8.0 (6.2-12.4) and 10.8 (7.1-16.7) months, respectively (NS). Resistance to tamoxifen was established only in 84%, 70% and 55% of patients in the three treatment arms, respectively. The median times from randomisation to resistance to tamoxifen were 12.5 (9.1-21.1), 13.2 (8.8-19.8) and 24.0 (16.9-60.9) months, respectively (p<0.001), without translation in differences in survival times.
Intermittent T or intermittent/alternated T and MPA had no impact on PFS or OS as compared with classical continuous T in patients with advanced breast cancer. Intermittent/alternated T and MPA resulted in prolonged time to resistance to T, but this might partly be due to bias by omittance of the proof of tamoxifen resistance in a high proportion of the patients in this treatment arm.
内分泌反应性肿瘤的持续配体耗竭可能会增强对治疗的抗性。他莫昔芬(T)间歇治疗被认为可模拟(不完全的)配体耗竭和重新引入。此外,有人推测他莫昔芬与一种非交叉耐药的内分泌治疗方式交替使用可(进一步)推迟激素抗性。
一线接受他莫昔芬治疗4个月后未进展的绝经后晚期乳腺癌患者被随机分组,分别继续接受他莫昔芬(每日40毫克)治疗、每两个月接受一次间歇他莫昔芬治疗或间歇/交替接受他莫昔芬和醋酸甲羟孕酮(MPA,每日300毫克)治疗。在停药期或接受MPA治疗期间病情进展时,应重新引入他莫昔芬。研究的终点为无进展生存期(PFS)、对他莫昔芬产生抗性的时间以及总生存期(OS)。
在593名登记患者中,276名被随机分组。经过8年随访,持续使用他莫昔芬、间歇使用他莫昔芬以及间歇/交替使用他莫昔芬和MPA的患者的中位PFS分别为11.0(8.1 - 15.2)、8.0(6.2 - 12.4)和10.8(7.1 - 16.7)个月(无显著差异)。在三个治疗组中,分别仅有84%、70%和55%的患者对他莫昔芬产生抗性。从随机分组到对他莫昔芬产生抗性的中位时间分别为12.5(9.1 - 21.1)、13.2(8.8 - 19.8)和24.0(16.9 - 60.9)个月(p<0.001),但生存期差异无统计学意义。
与晚期乳腺癌患者经典的持续使用他莫昔芬治疗相比,间歇使用他莫昔芬或间歇/交替使用他莫昔芬和MPA对PFS或OS均无影响。间歇/交替使用他莫昔芬和MPA可延长对他莫昔芬产生抗性的时间,但这可能部分归因于该治疗组中很大一部分患者未证实对他莫昔芬产生抗性所导致的偏差。
