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siAkt与紫杉醇序贯治疗对胃癌细胞系的影响。

Effects for Sequential Treatment of siAkt and Paclitaxel on Gastric Cancer Cell Lines.

作者信息

Ku Minhee, Kang Myounghwa, Suh Jin-Suck, Yang Jaemoon

机构信息

Department of Radiology, College of Medicine, Yonsei University, Seoul 03722, Republic of Korea;; Brain Korea 21 Plus Project for Medical Science, College of Medicine, Yonsei University, Seoul 03722, Republic of Korea;

Department of Radiology, College of Medicine, Yonsei University, Seoul 03722, Republic of Korea;

出版信息

Int J Med Sci. 2016 Sep 7;13(9):708-16. doi: 10.7150/ijms.15501. eCollection 2016.

Abstract

Real-time screening of cellular response on the drugs could provide valuable insights for the early detection of therapeutic efficiency and the evaluation of disease progression. Cancer cells have the ability to vary widely in response to stress in a manner to adjust the signaling pathway to promote the survival or having a resistance to stimulation. Cell-based label-free technologies using electronic impedance sensor have strategies for constructing the signature profiles of each cells. To achieve exquisite sensitivity to substantially change of live-cell response have an important role that predict the potential of therapeutic effects. In this study, we use an impedance-based real-time cell analysis system to investigate dynamic phenotypes of cells described as a cellular index value. We show that gastric cancer cells generated characteristic kinetic patterns that corresponded to the treatment order of therapeutics. The kinetic feature of the cells offers insightful information that cannot be acquired from a conventional single end-point assay. Furthermore, we employ a 'sequential treatment strategy' to increase cytotoxic effects with minimizing the use of chemotherapeutics. Specifically, treatment of paclitaxel (PTX) after down-regulating Akt gene expression using RNAi reduces the cell proliferation and increases apoptosis. We propose that the sequential treatment may exhibit more effective approach rather than traditional combination therapy. Moreover, the dynamic monitoring of cell-drug interaction enables us to obtain a better understanding of the temporal effects in vitro.

摘要

对药物的细胞反应进行实时筛选可为治疗效果的早期检测和疾病进展评估提供有价值的见解。癌细胞能够以调整信号通路以促进存活或产生刺激抗性的方式对应激做出广泛不同的反应。使用电阻抗传感器的无标记细胞技术具有构建每个细胞特征图谱的策略。实现对活细胞反应实质性变化的高灵敏度对于预测治疗效果的潜力具有重要作用。在本研究中,我们使用基于阻抗的实时细胞分析系统来研究被描述为细胞指数值的细胞动态表型。我们表明,胃癌细胞产生了与治疗药物的给药顺序相对应的特征动力学模式。细胞的动力学特征提供了从传统单终点分析中无法获得的有洞察力的信息。此外,我们采用“序贯治疗策略”以在尽量减少化疗药物使用的情况下增强细胞毒性作用。具体而言,在使用RNAi下调Akt基因表达后用紫杉醇(PTX)治疗可减少细胞增殖并增加细胞凋亡。我们提出序贯治疗可能比传统联合治疗表现出更有效的方法。此外,对细胞 - 药物相互作用的动态监测使我们能够更好地了解体外的时间效应。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/cd20/5027190/57722d6c3054/ijmsv13p0708g001.jpg

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