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利用进化原理延长乳腺癌临床前模型中的肿瘤控制时间。

Exploiting evolutionary principles to prolong tumor control in preclinical models of breast cancer.

作者信息

Enriquez-Navas Pedro M, Kam Yoonseok, Das Tuhin, Hassan Sabrina, Silva Ariosto, Foroutan Parastou, Ruiz Epifanio, Martinez Gary, Minton Susan, Gillies Robert J, Gatenby Robert A

机构信息

Department of Cancer Imaging and Metabolism, H. Lee Moffitt Cancer Center and Research Institute, Tampa, FL 33612, USA.

Department of Cancer Imaging and Metabolism, H. Lee Moffitt Cancer Center and Research Institute, Tampa, FL 33612, USA. Department of Physics, University of South Florida, Tampa, FL 33620, USA.

出版信息

Sci Transl Med. 2016 Feb 24;8(327):327ra24. doi: 10.1126/scitranslmed.aad7842.

Abstract

Conventional cancer treatment strategies assume that maximum patient benefit is achieved through maximum killing of tumor cells. However, by eliminating the therapy-sensitive population, this strategy accelerates emergence of resistant clones that proliferate unopposed by competitors-an evolutionary phenomenon termed "competitive release." We present an evolution-guided treatment strategy designed to maintain a stable population of chemosensitive cells that limit proliferation of resistant clones by exploiting the fitness cost of the resistant phenotype. We treated MDA-MB-231/luc triple-negative and MCF7 estrogen receptor-positive (ER(+)) breast cancers growing orthotopically in a mouse mammary fat pad with paclitaxel, using algorithms linked to tumor response monitored by magnetic resonance imaging. We found that initial control required more intensive therapy with regular application of drug to deflect the exponential tumor growth curve onto a plateau. Dose-skipping algorithms during this phase were less successful than variable dosing algorithms. However, once initial tumor control was achieved, it was maintained with progressively smaller drug doses. In 60 to 80% of animals, continued decline in tumor size permitted intervals as long as several weeks in which no treatment was necessary. Magnetic resonance images and histological analysis of tumors controlled by adaptive therapy demonstrated increased vascular density and less necrosis, suggesting that vascular normalization resulting from enforced stabilization of tumor volume may contribute to ongoing tumor control with lower drug doses. Our study demonstrates that an evolution-based therapeutic strategy using an available chemotherapeutic drug and conventional clinical imaging can prolong the progression-free survival in different preclinical models of breast cancer.

摘要

传统的癌症治疗策略假定,通过最大限度地杀死肿瘤细胞可使患者获得最大益处。然而,通过清除对治疗敏感的细胞群体,这种策略加速了耐药克隆的出现,这些克隆在没有竞争者的情况下增殖——这是一种被称为“竞争释放”的进化现象。我们提出了一种基于进化的治疗策略,旨在维持化学敏感细胞的稳定群体,通过利用耐药表型的适应性代价来限制耐药克隆的增殖。我们使用与磁共振成像监测的肿瘤反应相关的算法,用紫杉醇治疗在小鼠乳腺脂肪垫原位生长的MDA-MB-231/luc三阴性乳腺癌和MCF7雌激素受体阳性(ER(+))乳腺癌。我们发现,初始控制需要更密集的治疗,即定期给药,以使指数增长的肿瘤生长曲线转向平稳期。在此阶段,剂量跳过算法不如可变剂量算法成功。然而,一旦实现了初始肿瘤控制,就可以用逐渐减小的药物剂量维持。在60%至80%的动物中,肿瘤大小持续下降使得可以有长达数周的间隔期,在此期间无需治疗。对通过适应性治疗控制的肿瘤进行磁共振成像和组织学分析显示,血管密度增加且坏死减少,这表明由于肿瘤体积的强制稳定导致的血管正常化可能有助于用较低药物剂量持续控制肿瘤。我们的研究表明,使用一种现有的化疗药物和传统临床成像的基于进化的治疗策略可以延长不同乳腺癌临床前模型的无进展生存期。

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