Catania Chiara, Ascione Gilda, Adamoli Laura, De Pas Tommaso, Medici Marta, Franceschelli Lucia, Verri Elena, Magni Elena, Sanna Giuseppina, Torrisi Rosalba, Goldhirsch Aron, Nolè Franco
Unit for Medical Care, Division of Medical Oncology, European Institute of Oncology, 20141, Milan, Italy.
Breast Cancer Res Treat. 2007 Nov;106(1):97-103. doi: 10.1007/s10549-006-9481-8. Epub 2007 Jan 27.
Fulvestrant ('Faslodex') is an oestrogen receptor (ER) antagonist with no agonist effects. The drug was administered to heavily pre-treated patients with advanced breast cancer (ABC). Patients received Fulvestrant after disease progression (PD) on a previous endocrine treatment or as maintenance treatment after chemotherapy.
Fifty-seven postmenopausal women with ER and/or progesterone receptor-positive ABC resistant to previous endocrine treatments prospectively received fulvestrant 250 mg via intramuscular injection q 28.
Twenty-seven patients received fulvestrant after PD and 30 received it as maintenance therapy after chemotherapy. All patients received fulvestrant as second-up to eight-line endocrine treatment for ABC. One patient (2%) had a partial response (PR) and 24 patients (42%) had stable disease > or =12 weeks (SD), including 11 patients who had SD > or =24 weeks. Thirty-two patients (56%) had de novo PD. Clinical benefit (CB; PR + SD > or =24 weeks) occurred in 12 patients (21%). Patients treated as maintenance and treated upon PD had 0 and 4% PR, 43 and 41% SD (including 20 and 19% SD > or =24 weeks), 57 and 55% PD, respectively. Overall, median time to progression (TTP) was 3 months. No differences in CB rate (20% vs. 23%), TTP (3 months vs. 3 months) and time to treatment failure (3 months vs. 3 months) were observed between patients receiving fulvestrant as maintenance therapy and those treated at PD on prior endocrine treatment. No grade 2-4 NCI-CTC toxicity was recorded.
Fulvestrant treatment was associated with prolonged CB and was well tolerated in this group of heavily pre-treated patients with ABC. The outcomes appeared to be similar for patients treated upon PD and those receiving fulvestrant as maintenance therapy.
氟维司群(“芙仕得”)是一种无激动剂作用的雌激素受体(ER)拮抗剂。该药物用于接受过大量前期治疗的晚期乳腺癌(ABC)患者。患者在先前内分泌治疗疾病进展(PD)后或化疗后作为维持治疗接受氟维司群治疗。
57名绝经后ER和/或孕激素受体阳性且对先前内分泌治疗耐药的ABC患者前瞻性地接受了250mg氟维司群,每28天肌肉注射一次。
27名患者在PD后接受氟维司群治疗,30名患者在化疗后作为维持治疗接受该药物。所有患者均接受氟维司群作为ABC的二线至八线内分泌治疗。1名患者(2%)有部分缓解(PR),24名患者(42%)疾病稳定≥12周(SD),包括11名疾病稳定≥24周的患者。32名患者(56%)出现新发PD。12名患者(21%)出现临床获益(CB;PR+疾病稳定≥24周)。作为维持治疗和在PD时接受治疗的患者PR分别为0%和4%,疾病稳定分别为43%和41%(包括疾病稳定≥24周的20%和19%),PD分别为57%和55%。总体而言,中位进展时间(TTP)为3个月。接受氟维司群作为维持治疗的患者与在PD时接受先前内分泌治疗的患者在CB率(20%对23%)、TTP(3个月对3个月)和治疗失败时间(3个月对3个月)方面未观察到差异。未记录到2-4级美国国立癌症研究所常见毒性标准(NCI-CTC)毒性。
氟维司群治疗与延长的CB相关,并且在这组接受过大量前期治疗的ABC患者中耐受性良好。PD时接受治疗的患者与接受氟维司群作为维持治疗的患者的结果似乎相似。
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