随机 II 期研究评估帕博西尼联合来曲唑作为雌激素受体阳性早期乳腺癌新辅助治疗:PALLET 试验。
Randomized Phase II Study Evaluating Palbociclib in Addition to Letrozole as Neoadjuvant Therapy in Estrogen Receptor-Positive Early Breast Cancer: PALLET Trial.
机构信息
1 The Royal Marsden National Health Service Foundation Trust, London, United Kingdom.
2 Univeristy of Pittsburgh Medical Center Cancer Center, Pittsburgh, PA.
出版信息
J Clin Oncol. 2019 Jan 20;37(3):178-189. doi: 10.1200/JCO.18.01624. Epub 2018 Dec 6.
PURPOSE
CDK4/6 inhibitors are used to treat estrogen receptor (ER)-positive metastatic breast cancer (BC) in combination with endocrine therapy. PALLET is a phase II randomized trial that evaluated the effects of combination palbociclib plus letrozole as neoadjuvant therapy.
PATIENTS AND METHODS
Postmenopausal women with ER-positive primary BC and tumors greater than or equal to 2.0 cm were randomly assigned 3:2:2:2 to letrozole (2.5 mg/d) for 14 weeks (A); letrozole for 2 weeks, then palbociclib plus letrozole to 14 weeks (B); palbociclib for 2 weeks, then palbociclib plus letrozole to 14 weeks (C); or palbociclib plus letrozole for 14 weeks. Palbociclib 125 mg/d was administered orally on a 21-days-on, 7-days-off schedule. Core-cut biopsies were taken at baseline and 2 and 14 weeks. Coprimary end points for letrozole versus palbociclib plus letrozole groups (A v B + C + D) were change in Ki-67 (protein encoded by the MKI67 gene; immunohistochemistry) between baseline and 14 weeks and clinical response (ordinal and ultrasound) after 14 weeks. Complete cell-cycle arrest was defined as Ki-67 less than or equal to 2.7%. Apoptosis was characterized by cleaved poly (ADP-ribose) polymerase.
RESULTS
Three hundred seven patients were recruited. Clinical response was not significantly different between palbociclib plus letrozole and letrozole groups ( P = .20; complete response + partial response, 54.3% v 49.5%), and progressive disease was 3.2% versus 5.4%, respectively. Median log-fold change in Ki-67 was greater with palbociclib plus letrozole compared with letrozole (-4.1 v -2.2; P < .001) in the 190 evaluable patients (61.9%), corresponding to a geometric mean change of -97.4% versus -88.5%. More patients on palbociclib plus letrozole achieved complete cell-cycle arrest (90% v 59%; P < .001). Median log-fold change (suppression) of cleaved poly (ADP-ribose) polymerase was greater with palbociclib plus letrozole versus letrozole (-0.80 v -0.42; P < .001). More patients had grade 3 or greater toxicity on palbociclib plus letrozole (49.8% v 17.0%; P < .001) mainly because of asymptomatic neutropenia.
CONCLUSION
Adding palbociclib to letrozole significantly enhanced the suppression of malignant cell proliferation (Ki-67) in primary ER-positive BC, but did not increase the clinical response rate over 14 weeks, which was possibly related to a concurrent reduction in apoptosis.
目的
CDK4/6 抑制剂与内分泌治疗联合用于治疗雌激素受体(ER)阳性转移性乳腺癌(BC)。PALLET 是一项评估帕博西尼联合来曲唑作为新辅助治疗的 II 期随机试验。
患者和方法
绝经后 ER 阳性原发性 BC 且肿瘤大于或等于 2.0 cm 的患者随机分为 3:2:2:2 组,分别接受来曲唑(2.5 mg/d)治疗 14 周(A 组);来曲唑治疗 2 周,然后帕博西尼联合来曲唑治疗 14 周(B 组);帕博西尼治疗 2 周,然后帕博西尼联合来曲唑治疗 14 周(C 组);或帕博西尼联合来曲唑治疗 14 周。帕博西尼 125 mg/d 口服,21 天/周期,7 天/休息。基线和第 2、14 周时进行核心活检。来曲唑组与帕博西尼联合来曲唑组(A 组与 B+C+D 组)的主要终点是 Ki-67(MKI67 基因编码的蛋白;免疫组化)在基线至 14 周之间的变化以及 14 周后的临床反应(等级和超声)。完全细胞周期阻滞定义为 Ki-67 小于或等于 2.7%。凋亡通过 cleaved poly (ADP-ribose) polymerase 来表征。
结果
共招募了 307 名患者。帕博西尼联合来曲唑组与来曲唑组的临床反应无显著差异(P=0.20;完全缓解+部分缓解率分别为 54.3%和 49.5%),疾病进展率分别为 3.2%和 5.4%。190 名可评估患者(61.9%)中,与来曲唑相比,帕博西尼联合来曲唑组 Ki-67 的中位对数倍变化更大(-4.1 对-2.2;P<0.001),相应的几何平均变化为-97.4%对-88.5%。更多的患者达到完全细胞周期阻滞(90%对 59%;P<0.001)。与来曲唑相比,帕博西尼联合来曲唑组 cleaved poly (ADP-ribose) polymerase 的中位对数倍变化(抑制)更大(-0.80 对-0.42;P<0.001)。更多的患者在帕博西尼联合来曲唑组出现 3 级或更高级别的毒性(49.8%对 17.0%;P<0.001),主要是因为无症状性中性粒细胞减少。
结论
在 ER 阳性原发性 BC 中,与来曲唑联合使用帕博西尼可显著增强对恶性细胞增殖(Ki-67)的抑制作用,但在 14 周内并未增加临床反应率,这可能与凋亡的同时减少有关。
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