Abstract OT3-04-04: A randomized phase II study of pembrolizumab in combination with carboplatin versus carboplatin alone in breast cancer patients with chest wall disease, with immunologic and genomic correlative studies

N. Vidula, A. Goga, Jimmy Hwang, M. Liu, B. Park, R. Nanda, P. Pohlmann, A. Storniolo, A. Brufsky, V. Abramson, H. Rugo
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Abstract

Background: Thirty percent of patients with breast cancer may experience chest wall recurrence, which is associated with a higher risk of developing distant metastases and a poor prognosis. Cancer cells may evade immune rejection through the programmed cell death 1 (PD-1) pathway. Pembrolizumab, an anti-PD-1 antibody, binds PD-1 and inhibits its interaction with the programmed death ligand 1 (PD-L1) to facilitate tumor immune rejection. We hypothesize that pembrolizumab may be an effective therapy in chest wall recurrence, given the inflammatory nature, and the high expression of PD-1 in tumors with lymphovascular invasion. Platinum agents may enhance anti-tumor immunity in a synergistic manner, and the combination of pembrolizumab and carboplatin has demonstrated efficacy in advanced lung cancer. In this study, the combination of pembrolizumab and carboplatin is being evaluated in breast cancer patients with chest wall disease. Methods: This is a randomized phase II study of breast cancer patients with advanced, unresectable breast cancer involving the chest wall, being conducted through the Translational Breast Cancer Research Consortium (TBCRC). Patients may have hormone resistant disease (at least 2 prior lines of hormone therapy), triple negative breast cancer, or refractory HER2+ disease for enrollment. They may have other sites of distant metastases, have received any number of prior lines of therapy, have had prior surgery, but prior chest wall radiation is not necessary. Eighty-four patients at 7 TBCRC sites will be randomized 2:1 to treatment with pembrolizumab 200 mg IV and carboplatin AUC 5 IV every 3 weeks followed by pembrolizumab 200 mg IV alone every 3 weeks (Arm A, n=56) or carboplatin AUC 5 IV every 3 weeks (Arm B, n=28), with an option for patients in Arm B to cross-over to single agent pembrolizumab 200 mg IV every 3 weeks (arm Bx) on progression. Patients will undergo imaging with CT chest, abdomen, and pelvis at baseline and every 2 cycles of treatment for response evaluation. The primary endpoint is the disease control rate in the chest wall and distant sites at 18 weeks of treatment, and this study is powered to determine a 20% difference in disease control rates between arms A and B (hazard ratio of 0.52, α= 0.10, β= 0.20). After 18 patients are enrolled into Arm B, an interim analysis for futility will be conducted to enable early closure of that arm for lack of efficacy. Secondary endpoints in the study are toxicity, progression free survival, and response based on PD-L1 expression and irRECIST. Exploratory endpoints, which will be studied using peripheral blood testing and chest wall tumor biopsies at baseline and after 2 cycles of treatment, include determining associations of response with changes in tumor and peripheral blood immune composition, soluble PD-L1 expression, circulating tumor cells, cell free DNA, and tumor PD-L1 and MYC genomic expression. Ultimately this study promises to improve our understanding of checkpoint inhibition and chemotherapy for chest wall disease, and the underlying mechanism of action. This study is open for enrollment and 2 patients are currently enrolled. (NCT03095352). Citation Format: Vidula N, Goga A, Hwang J, Liu MC, Park BH, Nanda R, Pohlmann PR, Storniolo AM, Brufsky A, Abramson V, Rugo HS. A randomized phase II study of pembrolizumab in combination with carboplatin versus carboplatin alone in breast cancer patients with chest wall disease, with immunologic and genomic correlative studies [abstract]. In: Proceedings of the 2018 San Antonio Breast Cancer Symposium; 2018 Dec 4-8; San Antonio, TX. Philadelphia (PA): AACR; Cancer Res 2019;79(4 Suppl):Abstract nr OT3-04-04.
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OT3-04-04:一项随机II期研究,派姆单抗联合卡铂与单独卡铂治疗胸壁疾病乳腺癌患者,并进行免疫学和基因组相关研究
背景:30%的乳腺癌患者可能经历胸壁复发,这与发生远处转移和预后不良的高风险相关。癌细胞可能通过程序性细胞死亡1 (PD-1)途径逃避免疫排斥反应。Pembrolizumab是一种抗PD-1抗体,结合PD-1并抑制其与程序性死亡配体1 (PD-L1)的相互作用,促进肿瘤免疫排斥。我们假设pembrolizumab可能是胸壁复发的有效治疗方法,考虑到炎症性和淋巴血管侵袭肿瘤中PD-1的高表达。铂类药物可协同增强抗肿瘤免疫,派姆单抗与卡铂联合治疗晚期肺癌已证明有效。在这项研究中,正在评估派姆单抗和卡铂联合治疗胸壁疾病的乳腺癌患者。方法:这是一项随机II期研究,由乳腺癌转化研究联盟(TBCRC)进行,研究对象是晚期不可切除的累及胸壁的乳腺癌患者。入组的患者可能患有激素抵抗性疾病(至少有2个先前的激素治疗线)、三阴性乳腺癌或难治性HER2+疾病。他们可能有其他部位的远处转移,之前接受过各种治疗,之前做过手术,但之前胸壁放射治疗是不必要的。7个TBCRC部位的84名患者将被随机分为2:1,每3周接受派姆单抗200mg IV和卡铂AUC 5iv治疗,然后每3周单独使用派姆单抗200mg IV (A组,n=56)或每3周使用卡铂AUC 5iv (B组,n=28), B组的患者可以选择在进展时每3周使用单药派姆单抗200mg IV (Bx组)。患者将在基线和每2个治疗周期进行胸部、腹部和骨盆CT成像以评估疗效。主要终点是治疗18周时胸壁和远处部位的疾病控制率,该研究确定了a组和B组之间疾病控制率的20%差异(风险比为0.52,α= 0.10, β= 0.20)。在18例患者入组B组后,将进行无效的中期分析,以便在缺乏疗效的情况下尽早关闭该组。研究的次要终点是毒性、无进展生存期和基于PD-L1表达和irRECIST的反应。探索性终点将在基线和2个治疗周期后通过外周血检测和胸壁肿瘤活检进行研究,包括确定肿瘤和外周血免疫成分、可溶性PD-L1表达、循环肿瘤细胞、细胞游离DNA以及肿瘤PD-L1和MYC基因组表达的变化与疗效的关系。最终,这项研究有望提高我们对检查点抑制和胸壁疾病化疗的理解,以及潜在的作用机制。本研究开放入组,目前有2例患者入组。(NCT03095352)。引文格式:Vidula N, Goga A, Hwang J, Liu MC, Park BH, Nanda R, Pohlmann PR, Storniolo AM, Brufsky A, Abramson V, Rugo HS。一项随机II期研究,派姆单抗联合卡铂与单独卡铂治疗胸壁疾病乳腺癌患者,并进行免疫学和基因组相关研究[摘要]。2018年圣安东尼奥乳腺癌研讨会论文集;2018年12月4-8日;费城(PA): AACR;中国癌症杂志,2019;79(4增刊):OT3-04-04。
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