Pub Date : 2019-02-15DOI: 10.1158/1538-7445.SABCS18-OT2-09-02
Ps Thomas, Abu T. Patel, A. Contreras, Diane D. Liu, J. Lee, S. Khan, L. Vornik, E. Dimond, M. Perloff, B. Heckman-Stoddard, P. Brown
Background: Breast cancer prevention with anti-estrogens, including tamoxifen, raloxifene, and exemestane, has been shown to reduce the incidence of hormone receptor-positive breast cancer. However, agents that can reduce the incidence of hormone receptor negative breast cancer are currently lacking. Rexinoids such as bexarotene are vitamin A analogues that have been shown to be involved in cell differentiation, growth, and apoptosis. In preclinical mouse models that develop ER-negative breast cancers, bexarotene showed a significant reduction in mammary tumor development. Oral bexarotene has been evaluated in BRCA mutation carriers and significant decreases in cyclin D1 were noted in breast cells suggesting biological activity of bexarotene on breast tissue. Systemic side effects of hyperlipidemia and hypothyroidism were also found. Data from chemoprevention studies with topical 4-hydroxytamoxifen support the concept of topical agents penetrating into the breast tissue and exhibiting biological activity in the tissue. We hypothesize that topical bexarotene can be applied to the breast as a chemoprevention agent with penetration to the breast tissue without subsequent systemic side effects and toxicity as seen with oral bexarotene. Trial Design: Women at high risk for breast cancer will be recruited and assigned to one of three different dose levels: 10mg (1ml) every other day, 10mg (1ml) daily, 20mg (2ml) daily to one unaffected breast for 4 weeks. The primary endpoint of the study is to determine the recommended phase II dose of topical bexarotene 1% gel for evaluation in healthy at-risk women. Dose Limiting Toxicity (DLT) is defined as a grade 2 skin adverse event that persists for at least 6 days or any grade 3 or greater adverse event related to the study drug. A grade 2 skin adverse event that recurs and persists for at least 3 days is also a DLT. The Maximum Tolerated Dose (MTD) will be defined as the highest dose level at which no more than 2 participants experience a DLT among 10 participants treated. A conservative modification of the standard “3+3” design will be applied. The first three participants will be assigned to the lowest dose level. New cohorts of 3-4 participants will not be treated until toxicity has been fully evaluated for all current participants through 4 weeks. Once the MTD has been determined, an expansion cohort of an additional 10 patients will be recruited at the MTD to further evaluate safety and toxicity at this dose level as well bexarotene concentration in the breast tissue. Secondary endpoints include serum bexarotene level, tissue bexarotene levels, and changes in thyroid function tests, lipid profile, and calcium. The planned accrual for this study if maximally accrued to all dose levels and the dose expansion cohort will be 40 participants. Citation Format: Thomas PS, Patel AB, Contreras A, Liu DD, Lee JJ, Khan S, Vornik LA, Dimond EP, Perloff M, Heckman-Stoddard BM, Brown PH. A phase I dose escalation stud
背景:使用抗雌激素预防乳腺癌,包括他莫昔芬、雷洛昔芬和依西美坦,已被证明可以降低激素受体阳性乳腺癌的发生率。然而,目前缺乏能够降低激素受体阴性乳腺癌发病率的药物。类维生素A如贝沙罗汀是维生素A类似物,已被证明参与细胞分化、生长和凋亡。在发生er阴性乳腺癌的临床前小鼠模型中,贝沙罗汀显示出乳腺肿瘤发展的显著减少。口服贝沙罗汀对BRCA突变携带者进行了评估,发现乳腺细胞中细胞周期蛋白D1显著降低,表明贝沙罗汀对乳腺组织具有生物活性。还发现了高脂血症和甲状腺功能减退的全身副作用。外用4-羟他莫昔芬的化学预防研究数据支持外用药物穿透乳房组织并在组织中表现出生物活性的概念。我们假设局部贝沙罗汀可以作为化学预防剂应用于乳房,并渗透到乳房组织,而不会像口服贝沙罗汀那样产生全身副作用和毒性。试验设计:将招募乳腺癌高风险妇女,并将其分配到三种不同剂量水平中的一种:每隔一天10mg (1ml),每天10mg (1ml),每天20mg (2ml),持续4周。该研究的主要终点是确定1%贝沙罗汀凝胶在健康危险女性中的推荐II期剂量。剂量限制毒性(DLT)定义为持续至少6天的2级皮肤不良事件或与研究药物相关的任何3级或更大的不良事件。2级皮肤不良事件复发并持续至少3天也属于DLT。最大耐受剂量(MTD)将被定义为在10名接受治疗的参与者中不超过2名参与者经历DLT的最高剂量水平。将采用标准“3+3”设计的保守修改。前三位参与者将被分配到最低剂量水平。3-4名参与者的新队列将在4周内对所有当前参与者的毒性进行充分评估后才进行治疗。一旦确定了MTD,将在MTD招募另外10名患者的扩展队列,以进一步评估该剂量水平下的安全性和毒性以及乳房组织中的贝沙罗汀浓度。次要终点包括血清贝萨罗汀水平、组织贝萨罗汀水平、甲状腺功能测试、血脂和钙的变化。本研究的计划累积如果最大累积到所有剂量水平和剂量扩大队列将有40名参与者。引用格式:Thomas PS, Patel AB, Contreras A, Liu DD, Lee JJ, Khan S, Vornik LA, Dimond EP, Perloff M, Heckman-Stoddard BM, Brown PH.外用贝沙罗芬治疗乳腺癌高危女性的I期剂量增加研究[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):OT2-09-02。
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Pub Date : 2019-02-15DOI: 10.1158/1538-7445.sabcs18-ot1-01-06
O. Pagani, A. Partridge, F. Peccatori, H. Azim, M. Colleoni, C. Saura, J. Kroep, E. Warner, A. Gombos, AB Sætersdal, M. Ruggeri, R. Gelber, Z. Sun
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Pub Date : 2019-02-15DOI: 10.1158/1538-7445.SABCS18-OT1-12-02
Y. Ozaki, S. Kitano, Koji Matsumoto, Maiko Takahashi, T. Mukohara, M. Futamura, N. Masuda, J. Tsurutani, K. Yoshimura, H. Minami, T. Takano
Background : In recent years, anti-PD-1 antibody, an immune checkpoint inhibitor, has been developed for the treatment of various types of cancer, including breast cancer. Synergistic effects of nivolumab, paclitaxel and bevacizumab are expected, based on various preclinical data, when these drugs are administered in combination. A biomarker study is ongoing to evaluate the immune status of patients participating in the NEWBEAT trial, which is a phase II trial of nivolumab + paclitaxel + bevacizumab therapy as first-line treatment for patients with metastatic or recurrent HER2-negative breast cancer. Methods : HER2-negative breast cancer patients from the WJOG9917B (NEWBEAT) trial are enrolled in this biomarker study. To explore new biomarkers for combined treatment of breast cancer with immune-checkpoint inhibitors and anti-vascular endothelial growth factor antibodies, we propose to conduct multicolor immunohistochemistry (IHC) assays for immunomonitoring of the intra-tumor environment, such as the expressions of PD-L1, CD4 and CD8. Blood samples are collected before the start of treatment and at four time-points during the treatment, to determine, using a multicolor flow cytometry panel, the numbers of circulating immunosuppressive cells, such as regulatory T cells, myeloid-derived suppressor cells and tumor-associated macrophages (M2). In the NEWBEAT trial, patients receive nivolumab 240 mg/body on days 1 and 15, paclitaxel 90 mg/m2 on days 1, 8 and 15, and bevacizumab 10 mg/kg on days 1 and 15 every 4 weeks until disease progression. The primary endpoint is the objective response rate, and the key secondary endpoints include progression-free survival, overall survival, and toxicity of the protocol treatment. A total of 51 patients will be enrolled and the enrollment period will be one year. This trial opened to accrual in February 2018. Clinical trial registry number: UMIN000029590 Citation Format: Ozaki Y, Kitano S, Matsumoto K, Takahashi M, Mukohara T, Futamura M, Masuda N, Tsurutani J, Yoshimura K, Minami H, Takano T. Biomarker study of patients with HER2-negative metastatic breast cancer receiving combination therapy with nivolumab, bevacizumab and paclitaxel as first-line treatment (WJOG9917BTR) [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 OT1-12-02.
背景:近年来,抗pd -1抗体(一种免疫检查点抑制剂)已被开发用于治疗包括乳腺癌在内的各种类型的癌症。根据各种临床前数据,当这些药物联合使用时,预计纳武单抗、紫杉醇和贝伐单抗会产生协同效应。一项生物标志物研究正在进行中,以评估参加NEWBEAT试验的患者的免疫状态,该试验是一项将纳武单抗+紫杉醇+贝伐单抗治疗作为转移性或复发性her2阴性乳腺癌患者一线治疗的II期试验。方法:将WJOG9917B (NEWBEAT)试验中her2阴性的乳腺癌患者纳入这项生物标志物研究。为了探索新的生物标志物,联合免疫检查点抑制剂和抗血管内皮生长因子抗体治疗乳腺癌,我们建议进行多色免疫组织化学(IHC)检测肿瘤内环境的免疫监测,如PD-L1, CD4和CD8的表达。在治疗开始前和治疗期间的四个时间点采集血液样本,使用多色流式细胞仪检测循环免疫抑制细胞的数量,如调节性T细胞、髓源性抑制细胞和肿瘤相关巨噬细胞(M2)。在NEWBEAT试验中,患者在第1天和第15天接受纳武单抗240 mg/体,在第1、8和15天接受紫杉醇90 mg/m2,在第1天和第15天每4周接受贝伐单抗10 mg/kg,直到疾病进展。主要终点是客观缓解率,关键的次要终点包括无进展生存期、总生存期和方案治疗的毒性。共纳入51例患者,入组期为1年。该试验于2018年2月开始。临床试验注册号:UMIN000029590引用格式:Ozaki Y, Kitano S, Matsumoto K, Takahashi M, Mukohara T, Futamura M, Masuda N, Tsurutani J, Yoshimura K, Minami H, Takano T. her2阴性转移性乳腺癌患者纳武单抗、贝伐单抗和紫杉醇联合治疗的生物标志物研究(WJOG9917BTR)[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):1-12-02。
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Pub Date : 2019-02-15DOI: 10.1158/1538-7445.SABCS18-OT2-07-05
N. Masuda, T. Yamashita, S. Saji, K. Araki, Yoshinori Ito, T. Takano, M. Takahashi, J. Tsurutani, K. Koizumi, M. Kitada, Y. Kojima, Y. Sagara, H. Tada, T. Iwasa, T. Kadoya, T. Iwatani, H. Hasegawa, S. Morita, S. Ohno
Background: Docetaxel + Trastuzumab (H) + Pertuzumab (P) provided progression-free survival (PFS) and overall survival (OS) benefits in HER2-positive advanced or metastatic breast cancer (AMBC) in the CLEOPATRA study as a first-line therapy. However, long-term administration of docetaxel at a dose of 75 mg/m2 every 3 weeks in AMBC patients (pts) is difficult due to the toxicities. Eribulin mesylate (E) is a well-tolerated microtubule inhibitor, and we have reported the efficacy and safety of EHP regimen as first- and second-line therapy for AMBC in a multicenter, phase II study (JBCRG-M03/UMIN000012232). In this M06 study, we address the clinical question as to which is the better chemotherapy partner for HP as first line regimen, in terms of efficacy, toxicity and QOL. Methods: JBCRG-M06 is a multicenter open-label randomized phase III study for HER2-positive AMBC pts who have received no prior chemotherapy except for the HER2- Antibody-Drug Conjugate (ADC). Pts will be randomized 1:1 to E (1.4mg/m2 on day 1 and 8) + H (8 mg/kg loading dose followed by 6 mg/kg) +P (840 mg loading dose followed by 420 mg) q3wks or standard taxanes (docetaxel 75mg/m2 on day1 or paclitaxel 80mg/m2 on day 1, 8 and 15) + HP q3wks. Stratification factors for randomization are; presence of visceral metastases, number of prior taxanes on perioperative adjuvant treatment, and treatment with prior anti-HER2-ADC. Primary endpoint is PFS and secondary endpoints include overall response rate, duration of response, OS, patient-reported outcomes (PRO) relating to QOL and peripheral neuropathy, new-metastases free survival, and safety. Translational research to search for biomarker for individual precision therapy will be performed. Main eligibility criteria are as follows: pts with HER2-positive AMBC, female aged 20-70 years old, ECOG PS of 0-1, LVEF ≥ 50% at baseline and adequate organ function. Pts who had progressive MBC within 6 months after the end of primary adjuvant systemic chemotherapy are excluded. The sample size was calculated by type1 error (2-sided) of 0.05 and 80% power to estimate the noninferiority margin 1.33 with an expected median PFS of 14.2 months. The target number of pts is 480 recruited over the duration of 3-years. The first patient in was achieved on August 2017. (ClinicalTrials.gov Identifier:NCT03264547). Citation Format: Masuda N, Yamashita T, Saji S, Araki K, Ito Y, Takano T, Takahashi M, Tsurutani J, Koizumi K, Kitada M, Kojima Y, Sagara Y, Tada H, Iwasa T, Kadoya T, Iwatani T, Hasegawa H, Morita S, Ohno S. A phase III trial to compare eribulin mesylate + trastuzumab (H) + pertuzumab (P) with paclitaxel or docetaxel + HP for HER2-positive advanced or metastatic breast cancer (JBCRG-M06/ EMERALD) [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 OT2-07-05.
背景:在CLEOPATRA研究中,多西他赛+曲妥珠单抗(H) +帕妥珠单抗(P)作为一线治疗her2阳性晚期或转移性乳腺癌(AMBC)提供无进展生存期(PFS)和总生存期(OS)益处。然而,由于其毒性,AMBC患者(pts)很难以每3周75 mg/m2的剂量长期给予多西紫杉醇。甲磺酸埃瑞布林(E)是一种耐受性良好的微管抑制剂,我们已经在一项多中心II期研究中报道了EHP方案作为AMBC一线和二线治疗的有效性和安全性(JBCRG-M03/UMIN000012232)。在这项M06研究中,我们从疗效、毒性和生活质量方面探讨了HP作为一线方案的更好化疗伙伴的临床问题。方法:JBCRG-M06是一项多中心开放标签随机III期研究,针对HER2阳性AMBC患者,除HER2-抗体-药物偶联物(ADC)外未接受化疗。患者将按1:1的比例随机分配到E(第1天和第8天1.4mg/m2) + H (8 mg/kg负荷剂量后为6 mg/kg) +P (840 mg负荷剂量后为420 mg) q3周或标准紫杉醇(多西他赛75mg/m2第1天或紫杉醇80mg/m2第1、8和15天)+ HP q3周。随机化的分层因素有;内脏转移的存在,围手术期辅助治疗中既往紫杉烷类药物的数量,以及既往抗her2 - adc治疗。主要终点是PFS,次要终点包括总缓解率、缓解持续时间、OS、与生活质量和周围神经病变相关的患者报告结局(PRO)、无新转移生存期和安全性。将进行转化研究,寻找用于个体精准治疗的生物标志物。主要入选标准为:AMBC her2阳性,女性,年龄20-70岁,ECOG PS 0-1,基线时LVEF≥50%,脏器功能正常。在首次辅助全身化疗结束后6个月内发生进展性MBC的患者被排除在外。样本量计算采用1型误差(双侧)0.05和80%权数,估计非劣效性裕度为1.33,预期中位PFS为14.2个月。目标人数是在3年期间招募480人。第一位患者于2017年8月入院。(ClinicalTrials.gov标识符:NCT03264547)。引用格式:Masuda N, Yamashita T, Saji S, Araki K, Ito Y, Takano T, Takahashi M, Tsurutani J, Koizumi K, Kitada M, Kojima Y, Sagara Y, Tada H, Iwasa T, Kadoya T, Iwatani T, Hasegawa H, Morita S, Ohno S.与紫杉醇或多西紫杉醇+ HP治疗her2阳性晚期或转移性乳腺癌(JBCRG-M06/ EMERALD)的III期试验比较。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):OT2-07-05。
{"title":"Abstract OT2-07-05: A phase III trial to compare eribulin mesylate + trastuzumab (H) + pertuzumab (P) with paclitaxel or docetaxel + HP for HER2-positive advanced or metastatic breast cancer (JBCRG-M06/ EMERALD)","authors":"N. Masuda, T. Yamashita, S. Saji, K. Araki, Yoshinori Ito, T. Takano, M. Takahashi, J. Tsurutani, K. Koizumi, M. Kitada, Y. Kojima, Y. Sagara, H. Tada, T. Iwasa, T. Kadoya, T. Iwatani, H. Hasegawa, S. Morita, S. Ohno","doi":"10.1158/1538-7445.SABCS18-OT2-07-05","DOIUrl":"https://doi.org/10.1158/1538-7445.SABCS18-OT2-07-05","url":null,"abstract":"Background: Docetaxel + Trastuzumab (H) + Pertuzumab (P) provided progression-free survival (PFS) and overall survival (OS) benefits in HER2-positive advanced or metastatic breast cancer (AMBC) in the CLEOPATRA study as a first-line therapy. However, long-term administration of docetaxel at a dose of 75 mg/m2 every 3 weeks in AMBC patients (pts) is difficult due to the toxicities. Eribulin mesylate (E) is a well-tolerated microtubule inhibitor, and we have reported the efficacy and safety of EHP regimen as first- and second-line therapy for AMBC in a multicenter, phase II study (JBCRG-M03/UMIN000012232). In this M06 study, we address the clinical question as to which is the better chemotherapy partner for HP as first line regimen, in terms of efficacy, toxicity and QOL. Methods: JBCRG-M06 is a multicenter open-label randomized phase III study for HER2-positive AMBC pts who have received no prior chemotherapy except for the HER2- Antibody-Drug Conjugate (ADC). Pts will be randomized 1:1 to E (1.4mg/m2 on day 1 and 8) + H (8 mg/kg loading dose followed by 6 mg/kg) +P (840 mg loading dose followed by 420 mg) q3wks or standard taxanes (docetaxel 75mg/m2 on day1 or paclitaxel 80mg/m2 on day 1, 8 and 15) + HP q3wks. Stratification factors for randomization are; presence of visceral metastases, number of prior taxanes on perioperative adjuvant treatment, and treatment with prior anti-HER2-ADC. Primary endpoint is PFS and secondary endpoints include overall response rate, duration of response, OS, patient-reported outcomes (PRO) relating to QOL and peripheral neuropathy, new-metastases free survival, and safety. Translational research to search for biomarker for individual precision therapy will be performed. Main eligibility criteria are as follows: pts with HER2-positive AMBC, female aged 20-70 years old, ECOG PS of 0-1, LVEF ≥ 50% at baseline and adequate organ function. Pts who had progressive MBC within 6 months after the end of primary adjuvant systemic chemotherapy are excluded. The sample size was calculated by type1 error (2-sided) of 0.05 and 80% power to estimate the noninferiority margin 1.33 with an expected median PFS of 14.2 months. The target number of pts is 480 recruited over the duration of 3-years. The first patient in was achieved on August 2017. (ClinicalTrials.gov Identifier:NCT03264547). Citation Format: Masuda N, Yamashita T, Saji S, Araki K, Ito Y, Takano T, Takahashi M, Tsurutani J, Koizumi K, Kitada M, Kojima Y, Sagara Y, Tada H, Iwasa T, Kadoya T, Iwatani T, Hasegawa H, Morita S, Ohno S. A phase III trial to compare eribulin mesylate + trastuzumab (H) + pertuzumab (P) with paclitaxel or docetaxel + HP for HER2-positive advanced or metastatic breast cancer (JBCRG-M06/ EMERALD) [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 OT2-07-05.","PeriodicalId":19476,"journal":{"name":"Ongoing Clinical Trials","volume":"75 1","pages":""},"PeriodicalIF":0.0,"publicationDate":"2019-02-15","publicationTypes":"Journal Article","fieldsOfStudy":null,"isOpenAccess":false,"openAccessPdf":"","citationCount":null,"resultStr":null,"platform":"Semanticscholar","paperid":"74808898","PeriodicalName":null,"FirstCategoryId":null,"ListUrlMain":null,"RegionNum":0,"RegionCategory":"","ArticlePicture":[],"TitleCN":null,"AbstractTextCN":null,"PMCID":"","EPubDate":null,"PubModel":null,"JCR":null,"JCRName":null,"Score":null,"Total":0}
Pub Date : 2019-02-15DOI: 10.1158/1538-7445.SABCS18-OT2-01-03
Jae Seok Lee, H. Park, Joo Hang Kim, Dw Lee, Sy Song, D. Lew, J.-H. Kim, S. Kim, Y. Cho, H. Lee, Kb Lee, K. Yoon
{"title":"Abstract OT2-01-03: A prospective pilot study of simultaneous robotic assisted nipple sparing mastectomy and immediate reconstruction","authors":"Jae Seok Lee, H. Park, Joo Hang Kim, Dw Lee, Sy Song, D. Lew, J.-H. Kim, S. Kim, Y. Cho, H. Lee, Kb Lee, K. Yoon","doi":"10.1158/1538-7445.SABCS18-OT2-01-03","DOIUrl":"https://doi.org/10.1158/1538-7445.SABCS18-OT2-01-03","url":null,"abstract":"","PeriodicalId":19476,"journal":{"name":"Ongoing Clinical Trials","volume":"28 1","pages":""},"PeriodicalIF":0.0,"publicationDate":"2019-02-15","publicationTypes":"Journal Article","fieldsOfStudy":null,"isOpenAccess":false,"openAccessPdf":"","citationCount":null,"resultStr":null,"platform":"Semanticscholar","paperid":"84464792","PeriodicalName":null,"FirstCategoryId":null,"ListUrlMain":null,"RegionNum":0,"RegionCategory":"","ArticlePicture":[],"TitleCN":null,"AbstractTextCN":null,"PMCID":"","EPubDate":null,"PubModel":null,"JCR":null,"JCRName":null,"Score":null,"Total":0}
Pub Date : 2019-02-15DOI: 10.1158/1538-7445.sabcs18-ot2-04-04
J. Bazan, J. Stephens, D. Agnese, R. Skoracki, K. Arneson, J. Reiland, G. Gupta, K. Gallagher, S. McElroy, N. Gupta, J. White
{"title":"Abstract OT2-04-04: Multi-institution phase II trial of intraoperative electron beam radiotherapy boost at the time of breast conserving surgery with oncoplastic reconstruction in women with early-stage breast cancer","authors":"J. Bazan, J. Stephens, D. Agnese, R. Skoracki, K. Arneson, J. Reiland, G. Gupta, K. Gallagher, S. McElroy, N. Gupta, J. White","doi":"10.1158/1538-7445.sabcs18-ot2-04-04","DOIUrl":"https://doi.org/10.1158/1538-7445.sabcs18-ot2-04-04","url":null,"abstract":"","PeriodicalId":19476,"journal":{"name":"Ongoing Clinical Trials","volume":"48 1","pages":""},"PeriodicalIF":0.0,"publicationDate":"2019-02-15","publicationTypes":"Journal Article","fieldsOfStudy":null,"isOpenAccess":false,"openAccessPdf":"","citationCount":null,"resultStr":null,"platform":"Semanticscholar","paperid":"82159802","PeriodicalName":null,"FirstCategoryId":null,"ListUrlMain":null,"RegionNum":0,"RegionCategory":"","ArticlePicture":[],"TitleCN":null,"AbstractTextCN":null,"PMCID":"","EPubDate":null,"PubModel":null,"JCR":null,"JCRName":null,"Score":null,"Total":0}
Pub Date : 2019-02-15DOI: 10.1158/1538-7445.SABCS18-OT2-01-04
M. E. M. Noordaa, F. V. Duijnhoven, C. Loo, A. V. Loevezijn, E. Werkhoven, K. Vijver, T. Wiersma, H. Winter-Warnars, G. Sonke, M. Peeters
Background Improvements in neoadjuvant systemic therapy (NST) for breast cancer patients have led to increasing rates of pathologic complete response (pCR). Breast-conserving surgery (BCS) after NST is considered safe, despite the fact that the original tumor bed is not entirely excised. It can therefore be hypothesized that breast surgery could be omitted in patients achieving pCR. However, since imaging modalities are insufficiently accurate to predict pCR after NST, the need for surgery is unchanged. The MICRA trial is designed to determine the value of ultrasound guided biopsy of the breast in identifying pCR after NST. The ultimate aim of our study is to eliminate surgery of the breast in patients achieving pCR, consequently improving quality of life of these patients. Trial design The MICRA trial is a multi-center observational prospective cohort study. Inclusion and exclusion criteria are presented in table 1. In all patients receiving NST, a marker is placed in the center of the tumor area pre-NST. Magnetic resonance imaging (MRI) is performed pre-NST and just before or after the last course of NST. Patients with radiologic complete response (rCR; complete absence of pathologic contrast enhancement) or partial response (rPR, 0.1-2.0 cm residual contrast enhancement, ≥30% decrease in tumour size) are eligible for participation. In these patients, 8 ultrasound guided biopsies are obtained in the region surrounding the marker: 4 central ( Statistical analysis and accrual The primary endpoint of the trial is the false-negative rate (FNR) of the biopsy procedure. If the true FNR is 3%, 130 patients without pCR in specimen are sufficient to show that the FNR does not exceed 8% using a one-sided binomial test with a significance α-level of 0.05. With an expected average pCR rate of 65%, 375 patients with rCR will be included. In the rPR-group the expected pCR rate is 12% and therefore 150 patients will be included. In total 525 patients will be included. Until now, 144 patients have been included. Conclusion The ultimate aim of the MICRA trial is to eliminate surgery of the breast in patients achieving pCR, by identifying pCR with use of ultrasound guided biopsy. In this scenario, local therapy in patients with pCR would be restricted to radiotherapy. Citation Format: van der Noordaa ME, van Duijnhoven FH, Loo CE, van Loevezijn A, van Werkhoven E, van de Vijver KK, Wiersma T, Winter-Warnars HA, Sonke GS, Vrancken Peeters M-JT. Towards omitting breast cancer surgery in patients with pathologic complete response after neoadjuvant systemic therapy: The MICRA trial (minimally invasive complete response assessment) [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 OT2-01-04.
背景:乳腺癌患者的新辅助全身治疗(NST)的改进导致病理完全缓解(pCR)率的增加。NST后的保乳手术(BCS)被认为是安全的,尽管原来的肿瘤床没有完全切除。因此,可以假设在实现pCR的患者中可以省略乳房手术。然而,由于成像方式不足以准确预测NST后的pCR,因此手术的必要性没有改变。MICRA试验旨在确定超声引导乳腺活检在鉴别NST后pCR的价值。我们研究的最终目的是消除实现pCR患者的乳房手术,从而提高这些患者的生活质量。MICRA试验是一项多中心观察性前瞻性队列研究。纳入和排除标准见表1。在所有接受NST的患者中,在NST前肿瘤区域的中心放置一个标记物。磁共振成像(MRI)是在NST前、NST最后一个疗程之前或之后进行的。放射学完全缓解(rCR);完全没有病理对比增强)或部分缓解(rPR, 0.1-2.0 cm残留对比增强,肿瘤大小减小≥30%)符合参与条件。在这些患者中,在标记物周围区域进行了8次超声引导活检:4次中心(统计分析和累积)试验的主要终点是活检过程的假阴性率(FNR)。如果真实FNR为3%,则标本中无pCR的130例患者足以表明FNR不超过8%,采用单侧二项检验,显著性α-水平为0.05。预计平均pCR率为65%,将纳入375例rCR患者。在pCR组中,预期pCR率为12%,因此将纳入150例患者。总共525名患者将被纳入研究。到目前为止,已纳入144名患者。结论MICRA试验的最终目的是通过超声引导活检识别pCR,消除实现pCR患者的乳房手术。在这种情况下,pCR患者的局部治疗将仅限于放疗。引用格式:van der Noordaa ME, van Duijnhoven FH, Loo CE, van Loevezijn A, van Werkhoven E, van de Vijver KK, Wiersma T, Winter-Warnars HA, Sonke GS, Vrancken Peeters M-JT。新辅助全身治疗后病理完全缓解的乳腺癌患者免手术:MICRA试验(微创完全缓解评估)[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):OT2-01-04。
{"title":"Abstract OT2-01-04: Towards omitting breast cancer surgery in patients with pathologic complete response after neoadjuvant systemic therapy: The MICRA trial (minimally invasive complete response assessment)","authors":"M. E. M. Noordaa, F. V. Duijnhoven, C. Loo, A. V. Loevezijn, E. Werkhoven, K. Vijver, T. Wiersma, H. Winter-Warnars, G. Sonke, M. Peeters","doi":"10.1158/1538-7445.SABCS18-OT2-01-04","DOIUrl":"https://doi.org/10.1158/1538-7445.SABCS18-OT2-01-04","url":null,"abstract":"Background Improvements in neoadjuvant systemic therapy (NST) for breast cancer patients have led to increasing rates of pathologic complete response (pCR). Breast-conserving surgery (BCS) after NST is considered safe, despite the fact that the original tumor bed is not entirely excised. It can therefore be hypothesized that breast surgery could be omitted in patients achieving pCR. However, since imaging modalities are insufficiently accurate to predict pCR after NST, the need for surgery is unchanged. The MICRA trial is designed to determine the value of ultrasound guided biopsy of the breast in identifying pCR after NST. The ultimate aim of our study is to eliminate surgery of the breast in patients achieving pCR, consequently improving quality of life of these patients. Trial design The MICRA trial is a multi-center observational prospective cohort study. Inclusion and exclusion criteria are presented in table 1. In all patients receiving NST, a marker is placed in the center of the tumor area pre-NST. Magnetic resonance imaging (MRI) is performed pre-NST and just before or after the last course of NST. Patients with radiologic complete response (rCR; complete absence of pathologic contrast enhancement) or partial response (rPR, 0.1-2.0 cm residual contrast enhancement, ≥30% decrease in tumour size) are eligible for participation. In these patients, 8 ultrasound guided biopsies are obtained in the region surrounding the marker: 4 central ( Statistical analysis and accrual The primary endpoint of the trial is the false-negative rate (FNR) of the biopsy procedure. If the true FNR is 3%, 130 patients without pCR in specimen are sufficient to show that the FNR does not exceed 8% using a one-sided binomial test with a significance α-level of 0.05. With an expected average pCR rate of 65%, 375 patients with rCR will be included. In the rPR-group the expected pCR rate is 12% and therefore 150 patients will be included. In total 525 patients will be included. Until now, 144 patients have been included. Conclusion The ultimate aim of the MICRA trial is to eliminate surgery of the breast in patients achieving pCR, by identifying pCR with use of ultrasound guided biopsy. In this scenario, local therapy in patients with pCR would be restricted to radiotherapy. Citation Format: van der Noordaa ME, van Duijnhoven FH, Loo CE, van Loevezijn A, van Werkhoven E, van de Vijver KK, Wiersma T, Winter-Warnars HA, Sonke GS, Vrancken Peeters M-JT. Towards omitting breast cancer surgery in patients with pathologic complete response after neoadjuvant systemic therapy: The MICRA trial (minimally invasive complete response assessment) [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 OT2-01-04.","PeriodicalId":19476,"journal":{"name":"Ongoing Clinical Trials","volume":"40 1","pages":""},"PeriodicalIF":0.0,"publicationDate":"2019-02-15","publicationTypes":"Journal Article","fieldsOfStudy":null,"isOpenAccess":false,"openAccessPdf":"","citationCount":null,"resultStr":null,"platform":"Semanticscholar","paperid":"84652276","PeriodicalName":null,"FirstCategoryId":null,"ListUrlMain":null,"RegionNum":0,"RegionCategory":"","ArticlePicture":[],"TitleCN":null,"AbstractTextCN":null,"PMCID":"","EPubDate":null,"PubModel":null,"JCR":null,"JCRName":null,"Score":null,"Total":0}
Pub Date : 2019-02-15DOI: 10.1158/1538-7445.SABCS18-OT1-05-03
A. Kodera, K. Ogura, A. Hattori, H. Yukawa, Shiho Sakaguchi, A. Matsuoka, N. Tanaka, M. Kamimura, N. Jibiki, Y. Naritaka, A. Hirano
Background Chemotherapy for breast cancer causes alopecia as a side effect. Some patients refuse chemotherapy because of alopecia, resulting in the omission of a standard therapy. It is believed that a scalp cooling device can prevent alopecia by promoting vasoconstriction of the scalp and reducing exposure of the hair root cells to anticancer agents. There are phenotypic differences of the efficacy of a scalp cooling device for alopecia. In fact, a Dutch scalp cooling registry reported that the success rate of scalp cooling was 51% in European women and 33% in Asian women. Therefore, we aimed to investigate the efficacy of scalp cooling device for chemotherapy-induced alopecia among Asian women with breast cancer. Trial design This is a phase II trialto evaluate the efficacy and safety of scalp cooling device for risk reduction of alopecia in women with stage I/II/III breast cancer treated with adjuvant/neoadjuvant chemotherapy in a single institute. Eligibility criteria Women diagnosed with Stage I to III breast cancer who are scheduled to receive preoperative or postoperative adjuvant chemotherapy containing anthracycline and/or taxanes are enrolled. Patients who have blood malignancies (leukemia, non-Hodgkin lymphoma, other systemic lymphoma), and cold allergy, are excluded. Specific aims The primary endpoint is the proportion of patients with Common Terminology Criteria for Adverse Events (CTCAE) grade 0-1 alopecia after the completion of all cycles of chemotherapy (success rate). Secondary endpoints are safety, quality of life, use of wig or cap, and success rates after the completion of all cycles of chemotherapy distinguished by anthracycline(AC) and taxane. The cooling device is the Paxman scalp cooling system. Scalp cooling was performed from 30 mins before initiation until 90 mins (25 min for taxane) after chemotherapy. Pictures of the scalp were taken at the time of the initiation of each course. Statistical methods Successful treatment was defined as the presence of less than 50% of hair-loss area. The sample size was calculated using the Simon method, with a type I error of 10% (two-sided) and a study power of 80%.The expected success rate is 30%, with a threshold success rate of 10%, and the required number of patients was estimated to be 19. Present and target accrual Patient accrual was started in April 2018 and present accrual is 3. We plan to enroll a total of 20 patients in the trial. Citation Format: Kodera A, Ogura K, Hattori A, Yukawa H, Sakaguchi S, Matsuoka A, Tanaka N, Kamimura M, Jibiki N, Naritaka Y, Hirano A. Efficacy and safety of scalp cooling device for prevention of alopecia in patients with breast cancer [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 OT1-05-03.
背景:乳腺癌化疗的副作用是脱发。一些患者因为脱发而拒绝化疗,导致标准治疗的遗漏。据信,头皮冷却装置可以通过促进头皮血管收缩和减少发根细胞接触抗癌剂来预防脱发。头皮冷却装置对脱发的疗效存在表型差异。事实上,荷兰的一份头皮冷却登记报告称,欧洲女性头皮冷却的成功率为51%,亚洲女性为33%。因此,我们旨在研究头皮冷却装置对亚洲乳腺癌女性化疗性脱发的疗效。试验设计:这是一项II期试验,旨在评估头皮冷却装置在单个研究所辅助/新辅助化疗治疗的I/II/III期乳腺癌患者中降低脱发风险的有效性和安全性。入选标准诊断为1 - 3期乳腺癌的妇女,她们计划在术前或术后接受含有蒽环类药物和/或紫杉烷的辅助化疗。排除血液恶性肿瘤(白血病、非霍奇金淋巴瘤、其他系统性淋巴瘤)和感冒过敏的患者。主要终点是所有化疗周期完成后出现不良事件通用术语标准(CTCAE) 0-1级脱发的患者比例(成功率)。次要终点是安全性,生活质量,假发或帽的使用,以及以蒽环类药物(AC)和紫杉烷区分的所有化疗周期完成后的成功率。冷却装置为派克曼头皮冷却系统。开始前30分钟至化疗后90分钟(紫杉烷为25分钟)进行头皮冷却。在每个疗程开始时拍摄头皮照片。治疗成功的标准是脱发面积小于50%。样本量采用Simon方法计算,I型误差为10%(双侧),研究功率为80%。预期成功率为30%,阈值成功率为10%,所需患者数估计为19例。当前和目标收益患者收益于2018年4月开始,当前收益为3。我们计划在试验中总共招募20名患者。引用格式:Kodera, Ogura K, Hattori A, Yukawa H, Sakaguchi S, Matsuoka A, Tanaka N, Kamimura M, Jibiki N, Naritaka Y, Hirano A.头皮冷却装置预防乳腺癌患者脱发的疗效和安全性[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):01-05-03。
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Pub Date : 2019-02-15DOI: 10.1158/1538-7445.SABCS18-OT1-01-07
S. Kumar, J. Benson, S. McIntosh, P. King, G. Dougall, A. Kateb, A. Vallier, L. Jones, W. Qian, E. Provenzano, C. Caldas, P. Pantziarka, J. Carroll, R. Baird
Background: Published preclinical findings provided new insights into the functional 9cross-talk9 between the oestrogen receptor (ER) and the progesterone receptor (PR) in breast cancer (BC) (Mohammed et al., Nature, 2015). Addition of a PR agonist to anti-oestrogens directly modifies ERa chromatin binding and the transcriptional response in breast cancer cells, and is anti-proliferative in vitro and in vivo . Megestrol Acetate (MA), an off-patent semi-synthetic derivative of progesterone, has been licensed for many years as treatment for ER+ metastatic BC. There is also good evidence for the effectiveness of MA as a supportive therapy to ameliorate endocrine therapy-related hot flushes. Trial design: PIONEER is a three-arm, open label, multi-centre randomized phase II pre-surgical window trial evaluating effects of 15 days of preoperative therapy with Letrozole (LET), or LET plus MA 40mg, or LET plus MA 160mg in postmenopausal women with ER+ HER2- invasive primary BC. Eligibility criteria: Inclusion Criteria Postmenopausal women with histologically confirmed invasive BC, ≥T1c, clinical NX or N0-N3, ER+ (Allred≥3), and HER2- 2 groups of patients are potentially eligible: Cohort A: Patients whose cancers have been deemed to be operable by the Multi-Disciplinary Team (MDT) with surgery planned for the next 2-6 weeks Cohort B: Patients with early or locoregionally advanced BC planned for primary endocrine therapy either in lieu of surgery or as neoadjuvant therapy before surgery� ECOG performance status of 0-2 Adequate Liver, Renal, Bone marrow function Exclusion Criteria Hormone replacement therapy in the last 6 months Treatment with tamoxifen or an aromatase inhibitor (AI) in the last 6 months A progestogen-containing intrauterine system in situ, unless removed prior to randomisation Metastatic disease on presentation Recurrent BC (patients with a new primary invasive BC are eligible) S p ecific aims: The primary endpoint is % change in proliferation between baseline and day 15 tumor biopsies, measured by Ki67 IHC assessment. Secondary endpoints include: expression of Aurora Kinase A, Caspase 3 and AR/PR/EMT markers by IHC; and safety endpoints. Exploratory endpoints: transcription factor mapping (ChIP-seq) and identification of differential ERa-associated proteins (RIME) on paired fresh-frozen tumor samples. PIONEER will help determine whether there is value in conducting a Phase III adjuvant study to investigate the longer term benefit of combining an AI with MA, and if so, at what dose (40mg vs. 160mg). Statistical methods: Patients are randomized in a 1:1.5:1.5 ratio into arms A:B:C. Based on results from previous clinical trials, a mean 66% reduction in Ki67 is anticipated for LET alone (arm A), and a 77.5% reduction for the combination arms B and C, based on preclinical data. Present and target accrual: Patients are being recruited in Cambridge, Cornwall, Belfast & London with 6 other UK sites due to open q3/4 2018. At the time of submission
背景:已发表的临床前研究结果为乳腺癌(BC)中雌激素受体(ER)和孕激素受体(PR)之间的功能性交叉对话提供了新的见解(Mohammed et al., Nature, 2015)。在抗雌激素中加入PR激动剂可直接改变乳腺癌细胞中的ERa染色质结合和转录反应,并在体外和体内具有抗增殖作用。醋酸甲地孕酮(MA)是一种未获专利的孕酮半合成衍生物,多年来一直被许可用于ER+转移性BC的治疗。也有很好的证据表明,MA作为一种支持治疗的有效性,以改善内分泌治疗相关的潮热。试验设计:PIONEER是一项三组、开放标签、多中心随机II期术前窗口试验,评估绝经后ER+ HER2侵袭性原发性乳腺癌患者术前15天来曲唑(LET)、LET + MA 40mg或LET + MA 160mg治疗的效果。绝经后经组织学证实浸润性BC,≥T1c,临床NX或N0-N3, ER+ (Allred≥3)和HER2- 2组患者可能符合条件:队列A:多学科团队(MDT)认为癌症可手术,计划在未来2-6周进行手术的患者早期或局部进展性BC患者术前计划进行初级内分泌治疗替代手术或作为新辅助治疗ECOG表现0-2肝、肾、骨髓功能正常排除标准最近6个月激素替代治疗最近6个月使用他莫昔芬或芳香化酶抑制剂(AI)原位含孕激素宫内系统除非在随机化之前切除转移性疾病复发性BC(新的原发性浸润性BC患者符合条件)S p特定目的:主要终点是基线和第15天肿瘤活检之间增殖变化的百分比,通过Ki67 IHC评估测量。次要终点包括:IHC中极光激酶A、Caspase 3和AR/PR/EMT标志物的表达;还有安全端点。探索终点:转录因子定位(ChIP-seq)和鉴定配对新鲜冷冻肿瘤样品上的差异era相关蛋白(RIME)。PIONEER将帮助确定进行III期辅助研究是否有价值,以调查AI与MA联合使用的长期益处,如果有,剂量是多少(40mg vs 160mg)。统计学方法:将患者按1:1.5:1.5的比例随机分为a:B:C组。根据先前的临床试验结果,根据临床前数据,预计单独使用LET (a组)的Ki67平均降低66%,联合使用B和C组的Ki67平均降低77.5%。目前和目标收益:在剑桥、康沃尔、贝尔法斯特和伦敦招募患者,其他6个英国站点将于2018年3/4季度开放。在提交时,已经招募了29名患者。总共需要招募189名患者。引文格式:Kumar SS, Benson J, McIntosh S, King P, Dougall G, Kateb A, Vallier A-L, Jones L, Qian W, Provenzano E, Caldas C, Pantziarka P, Carroll J, Baird RD. PIONEER-绝经后雌激素受体阳性乳腺癌患者来曲唑联合PR受体拮抗剂乙酸甲地孕酮的术前窗口研究[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):01- 01-07。
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Pub Date : 2019-02-15DOI: 10.1158/1538-7445.SABCS18-OT3-04-04
N. Vidula, A. Goga, Jimmy Hwang, M. Liu, B. Park, R. Nanda, P. Pohlmann, A. Storniolo, A. Brufsky, V. Abramson, H. Rugo
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
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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