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Dual Drug Conjugated Nanoparticle for Simultaneous Targeting of Mitochondria and Nucleus in Cancer Cells

机译:双药物共轭纳米粒子同时靶向线粒体和细胞核在癌细胞中。

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Effective targeting of mitochondria has emerged as an alternative strategy in cancer chemotherapy. However, considering mitochondrias crucial role in cellular energetics, metabolism and signaling, targeting mitochondria with small molecules would lead to severe side effects in cancer patients. Moreover, mitochondrial functions are highly dependent on other cellular organelles like nucleus. Hence, simultaneous targeting of mitochondria and nucleus could lead to more effective anticancer strategy. To achieve this goal, we have developed sub 200 nm particles from dual drug conjugates derived from direct tethering of mitochondria damaging drug (alpha-tocopheryl succinate) and nucleus damaging drugs (cisplatin, doxorubicin and paclitaxel). These dual drug conjugated nanoparticles were internalized into the acidic lysosomal compartments of the HeLa cervical cancer cells through endocytosis and induced apoptosis through cell cycle arrest. These nanoparticles damaged mitochondrial morphology and triggered the release of cytochrome c. Furthermore, these nanoparticles target nucleus to induce DNA damage, fragment the nuclear morphology and damage the cytoskeletal protein tubulin. Therefore, these dual drug conjugated nanoparticles can be successfully used as a platform technology for simultaneous targeting of multiple subcellular organelles in cancer cells to improve the therapeutic efficacy of the free drugs.
机译:线粒体的有效靶向已成为癌症化学疗法的替代策略。然而,考虑到线粒体在细胞能量,代谢和信号传导中的关键作用,以小分子靶向线粒体将导致癌症患者严重的副作用。此外,线粒体功能高度依赖于其他细胞器,如细胞核。因此,同时靶向线粒体和细胞核可能导致更有效的抗癌策略。为实现此目标,我们从线粒体破坏性药物(琥珀酸α-生育酚酯)和细胞核破坏性药物(顺铂,阿霉素和紫杉醇)的直接束缚中获得了双重药物结合物的亚200 nm颗粒。这些双重药物结合的纳米颗粒通过内吞作用被内化到HeLa宫颈癌细胞的酸性溶酶体区室中,并通过细胞周期停滞诱导凋亡。这些纳米颗粒破坏了线粒体的形态并触发了细胞色素c的释放。此外,这些纳米颗粒靶向细胞核,以诱导DNA损伤,使核形态断裂,并损伤细胞骨架蛋白微管蛋白。因此,这些双重药物缀合的纳米颗粒可以成功地用作同时靶向癌细胞中多个亚细胞器以改善游离药物的治疗功效的平台技术。

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