摘要:外用贝沙罗汀治疗乳腺癌高危女性的I期剂量递增研究

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
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引用次数: 1

摘要

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。
本文章由计算机程序翻译,如有差异,请以英文原文为准。
Abstract OT2-09-02: A phase I dose escalation study of topical bexarotene in women at high risk for breast cancer
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 study of topical bexarotene in women at high risk for 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 OT2-09-02.
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