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A highly selective dual-therapeutic nanosystem for simultaneous anticancer and antiangiogenesis therapy

机译:一种高精度的双治疗纳米系统,用于同时抗癌和抗脑发生治疗

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摘要

The rational design of highly selective and cancer-targeted nanodrug delivery systems with attractive anticancer activities is urgently needed for future exploration and translational application of nano-medicine. As angiogenesis and tumor growth could be mutually enhanced, dual therapeutic nanomedicine with simultaneous antiangiogenesis and anticancer activities is practical for cancer therapy. Therefore, herein we have rationally designed functionalized mesoporous silica nanoparticles (MSNs) to realize the dual therapy of tumor growth and angiogenesis based on the biochemical similarity of membranes of cancer cells and angiogenic cells. This nanosystem demonstrates high selectivity in vivo against cancer cells with high integrin expression levels in two-tumor bearing models, and could simultaneously inhibit cancer cell growth and disrupt tumor neovasculature, thus achieving satisfactory in vivo anticancer efficacy. Interestingly, the nanosystem triggers ROS overproduction in both cancer and human umbilical vein endothelial cells, which activates various downstream signaling pathways to regulate cell cycle arrest and apoptosis. Moreover, the nanosystem also effectively reduces the toxic side effects of loaded drugs to normal tissues and prolongs blood circulation in vivo. Therefore, this study provides a simple approach for facile manufacture of a potent nanodrug delivery system that could achieve dual therapy of tumor growth and angiogenesis.
机译:纳米医药的未来勘探和翻译应用,迫切需要具有吸引力的抗癌活动的高选择性和癌症靶向纳米树脂输送系统的理性设计。由于血管生成和肿瘤生长可以相互增强,具有同时抗脑发生和抗癌活动的双治疗纳米胺对于癌症治疗是实用的。因此,在本文中,我们具有基于癌细胞和血管生成细胞的膜的生化相似性来实现官能化的中孔硅纳米粒子(MSNS)以实现肿瘤生长和血管生成的双重治疗。该纳米系统在两种肿瘤轴承模型中具有高整联蛋白表达水平的体内对癌细胞的高选择性,并且可以同时抑制癌细胞生长和破坏肿瘤新生动物,从而达到体内抗癌疗效的令人满意。有趣的是,纳米系统在癌症和人脐静脉内皮细胞中触发ROS过量生产,其激活各种下游信号传导途径以调节细胞周期停滞和细胞凋亡。此外,纳米系统还有效地降低了装载药物对正常组织的毒副作用,延长体内血液循环。因此,本研究提供了一种简单的方法,用于容纳有效的纳米树脂递送系统的制造,可以实现肿瘤生长和血管生成的双重治疗。

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