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FUCCI Real-Time Cell-Cycle Imaging as a Guide for Designing Improved Cancer Therapy: A Review of Innovative Strategies to Target Quiescent Chemo-Resistant Cancer Cells

机译:FUCCI实时细胞周期成像作为设计改善的癌症治疗的指导:对靶向静态化疗癌细胞的创新策略综述

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摘要

Progress in chemotherapy of solid cancer has been tragically slow due, in large part, to the chemoresistance of quiescent cancer cells in tumors. The fluorescence ubiquitination cell-cycle indicator (FUCCI) was developed in 2008 by Miyawaki et al., which color-codes the phases of the cell cycle in real-time. FUCCI utilizes genes linked to different color fluorescent reporters that are only expressed in specific phases of the cell cycle and can, thereby, image the phases of the cell cycle in real-time. Intravital real-time FUCCI imaging within tumors has demonstrated that an established tumor comprises a majority of quiescent cancer cells and a minor population of cycling cancer cells located at the tumor surface or in proximity to tumor blood vessels. In contrast to most cycling cancer cells, quiescent cancer cells are resistant to cytotoxic chemotherapy, most of which target cells in S/G2/M phases. The quiescent cancer cells can re-enter the cell cycle after surviving treatment, which suggests the reason why most cytotoxic chemotherapy is often ineffective for solid cancers. Thus, quiescent cancer cells are a major impediment to effective cancer therapy. FUCCI imaging can be used to effectively target quiescent cancer cells within tumors. For example, we review how FUCCI imaging can help to identify cell-cycle-specific therapeutics that comprise decoy of quiescent cancer cells from G1 phase to cycling phases, trapping the cancer cells in S/G2 phase where cancer cells are mostly sensitive to cytotoxic chemotherapy and eradicating the cancer cells with cytotoxic chemotherapy most active against S/G2 phase cells. FUCCI can readily image cell-cycle dynamics at the single cell level in real-time in vitro and in vivo. Therefore, visualizing cell cycle dynamics within tumors with FUCCI can provide a guide for many strategies to improve cell-cycle targeting therapy for solid cancers.
机译:在实体癌的化学疗法的进展一直可悲缓慢​​由于,在很大程度上,静态癌细胞在肿瘤中的化学抗性。荧光泛素化细胞周期指示符(FUCCI)通过胁等人,在2008年开发出的颜色代码在实时的细胞周期的阶段。 FUCCI利用连接到不同颜色的荧光记者基因只在细胞周期和CAN的特定阶段表达,从而,图像细胞周期的实时的阶段。肿瘤内活实时FUCCI成像已经证明,已建立的肿瘤包括占多数的静态癌细胞和循环位于肿瘤表面或邻近肿瘤血管的癌细胞的一小群。与大多数循环癌细胞,静态癌细胞对细胞毒性化疗有抗性,其中大部分在S / G2 / M期的靶细胞。幸存的治疗,这说明了为什么大多数细胞毒性化疗往往无效固体癌症的原因后,静态癌细胞可以重新进入细胞周期。因此,静态癌细胞是一个主要障碍有效的癌症疗法。 FUCCI成像可用于有效地定位在肿瘤内的静态癌细胞。例如,我们审查FUCCI成像可以如何帮助识别细胞周期特异性疗法静态癌细胞从G1期到循环阶段,处于S捕集癌细胞/ G2相,其中癌细胞是细胞毒性化疗大多敏感的包含诱饵和消除癌细胞与细胞毒性化疗针对S / G2期的细胞最活跃的。 FUCCI可以在体外和体内实时单细胞水平上容易地图像细胞周期动力学。因此,FUCCI肿瘤内可视化细胞周期动力学可以提供指南许多策略来提高对实体癌细胞周期靶向疗法。

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