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首页> 外文期刊>Nature biotechnology >Drug sensitivity of single cancer cells is predicted by changes in mass accumulation rate
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Drug sensitivity of single cancer cells is predicted by changes in mass accumulation rate

机译:单个癌细胞的药物敏感性通过质量累积率的变化预测

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Assays that can determine the response of tumor cells to cancer therapeutics could greatly aid the selection of drug regimens for individual patients. However, the utility of current functional assays is limited, and predictive genetic biomarkers are available for only a small fraction of cancer therapies. We found that the single-cell mass accumulation rate (MAR), profiled over many hours with a suspended microchannel resonator, accurately defined the drug sensitivity or resistance of glioblastoma and B-cell acute lymphocytic leukemia cells. MAR revealed heterogeneity in drug sensitivity not only between different tumors, but also within individual tumors and tumor-derived cell lines. MAR measurement predicted drug response using samples as small as 25 ml of peripheral blood while maintaining cell viability and compatibility with downstream characterization. MAR measurement is a promising approach for directly assaying single-cell therapeutic responses and for identifying cellular subpopulations with phenotypic resistance in heterogeneous tumors.
机译:可以确定肿瘤细胞对癌症治疗药物反应的测定方法,可以极大地帮助为个别患者选择药物治疗方案。然而,当前功能测定的用途是有限的,并且预测性遗传生物标记仅可用于一小部分癌症治疗。我们发现,使用悬浮微通道共振器经过多个小时进行分析的单细胞质量累积率(MAR)准确定义了胶质母细胞瘤和B细胞急性淋巴细胞白血病的药物敏感性或耐药性。 MAR揭示了不仅在不同肿瘤之间,而且在单个肿瘤和肿瘤来源的细胞系中,药物敏感性的异质性。 MAR测量使用小至25 ml的外周血样本预测药物反应,同时保持细胞活力和与下游特征的相容性。 MAR测量是一种有前途的方法,可以直接检测单细胞治疗反应并鉴定异质性肿瘤中具有表型抗性的细胞亚群。

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