活性氧介导维甲酸联合微管抑制剂ABT-751对多药耐药复发性神经母细胞瘤异种移植瘤的协同活性。
Reactive Oxygen Species Mediates the Synergistic Activity of Fenretinide Combined with the Microtubule Inhibitor ABT-751 against Multidrug-Resistant Recurrent Neuroblastoma Xenografts.
作者信息
Chen Nancy E, Maldonado N Vanessa, Khankaldyyan Vazgen, Shimada Hiroyuki, Song Michael M, Maurer Barry J, Reynolds C Patrick
机构信息
Department of Systems, Biology, and Disease, University of Southern California School of Medicine, Los Angeles, California.
Department of Pediatrics, Children's Hospital Los Angeles, Los Angeles, California.
出版信息
Mol Cancer Ther. 2016 Nov;15(11):2653-2664. doi: 10.1158/1535-7163.MCT-16-0156. Epub 2016 Aug 16.
ABT-751 is a colchicine-binding site microtubule inhibitor. Fenretinide (4-HPR) is a synthetic retinoid. Both agents have shown activity against neuroblastoma in laboratory models and clinical trials. We investigated the antitumor activity of 4-HPR + the microtubule-targeting agents ABT-751, vincristine, paclitaxel, vinorelbine, or colchicine in laboratory models of recurrent neuroblastoma. Drug cytotoxicity was assessed in vitro by a fluorescence-based assay (DIMSCAN) and in subcutaneous xenografts in nu/nu mice. Reactive oxygen species levels (ROS), apoptosis, and mitochondrial depolarization were measured by flow cytometry; cytochrome c release and proapoptotic proteins were measured by immunoblotting. 4-HPR + ABT-751 showed modest additive or synergistic cytotoxicity, mitochondrial membrane depolarization, cytochrome c release, and caspase activation compared with single agents in vitro; synergism was inhibited by antioxidants (ascorbic acid, α-tocopherol). 4-HPR + ABT-751 was highly active against four xenograft models, achieving multiple maintained complete responses. The median event-free survival (days) for xenografts from 4 patients combined was control = 28, 4-HPR = 49, ABT-751 = 77, and 4-HPR + ABT-751 > 150 (P < 0.001). Apoptosis (terminal deoxynucleotidyl transferase-mediated dUTP nick end labeling, TUNEL) was significantly higher in 4-HPR + ABT-751-treated tumors than with single agents (P < 0.01) and was inhibited by ascorbic acid and α-tocopherol (P < 0.01), indicating that ROS from 4-HPR enhanced the activity of ABT-751. 4-HPR also enhanced the activity against neuroblastoma xenografts of vincristine or paclitaxel, but the latter combinations were less active than 4-HPR + ABT-751. Our data support clinical evaluation of 4-HPR combined with ABT-751 in recurrent and refractory neuroblastoma. Mol Cancer Ther; 15(11); 2653-64. ©2016 AACR.
ABT - 751是一种结合秋水仙碱位点的微管抑制剂。芬维A胺(4 - HPR)是一种合成类视黄醇。在实验室模型和临床试验中,这两种药物均已显示出对神经母细胞瘤的活性。我们在复发性神经母细胞瘤的实验室模型中研究了4 - HPR与靶向微管药物ABT - 751、长春新碱、紫杉醇、长春瑞滨或秋水仙碱联合使用的抗肿瘤活性。通过基于荧光的检测方法(DIMSCAN)在体外评估药物细胞毒性,并在无胸腺裸鼠的皮下异种移植瘤中进行评估。通过流式细胞术测量活性氧水平(ROS)、细胞凋亡和线粒体去极化;通过免疫印迹法测量细胞色素c释放和促凋亡蛋白。与单一药物相比,4 - HPR + ABT - 751在体外显示出适度的相加或协同细胞毒性、线粒体膜去极化、细胞色素c释放和半胱天冬酶激活;抗氧化剂(抗坏血酸、α - 生育酚)可抑制协同作用。4 - HPR + ABT - 751对四种异种移植瘤模型具有高度活性,实现了多次持续的完全缓解。来自4例患者的异种移植瘤的无事件生存期中位数(天)为:对照组 = 28,4 - HPR = 49,ABT - 751 = 77,4 - HPR + ABT - 751 > 150(P < 0.001)。在4 - HPR + ABT - 751治疗的肿瘤中,细胞凋亡(末端脱氧核苷酸转移酶介导的dUTP缺口末端标记,TUNEL)显著高于单一药物治疗组(P < 0.01),且被抗坏血酸和α - 生育酚抑制(P < 0.01),表明4 - HPR产生的ROS增强了ABT - 751的活性。4 - HPR还增强了长春新碱或紫杉醇对神经母细胞瘤异种移植瘤的活性,但后两者联合用药的活性低于4 - HPR + ABT - 751。我们的数据支持对4 - HPR联合ABT - 751用于复发性和难治性神经母细胞瘤进行临床评估。《分子癌症治疗》;15(11);2653 - 64。©2016美国癌症研究协会。
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