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A microchip for integrated single-cell genotoxicity assay

机译:用于集成单细胞遗传毒性测定的微芯片

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With the development of large-scale biologic databases, precision medicine is becoming a frontier in biomedical research. As a main focus of precision medicine study, cancer has been widely accepted as a disease born out of inherited genetic variations or accumulating genomic damage. At the single-cell level, microfluidics or lab-on-a chip technology for cancer study is an emerging tool for improving risk assessment, diagnostic categories and therapeutic strategies. This work presents a multi-layer microchip for single-cell gene expression profiling. Treated by three drug reagents (i.e. methyl methanesulfonate, docetaxel and colchicine) with varied concentrations and time lengths, individual human breast cancer cells (MCF-7) are then lysed on-chip, and the released mRNA templates are captured and reversely transcribed into cDNA on microbead surface. Three genes (GAPDH, CDKN1A, AURKA) are amplified and quantified simultaneously through triplex real-time polymerase chain reactions (qPCR). Readout per run is set to be eighteen, and can be further improved following same approach. The microchip is able to integrate all steps of single-cellgene expression profiling, and provide precision study of drug induced genotoxicity with reduced reagents consumption per reaction and instrumental cost.
机译:随着大规模生物数据库的发展,精密医学正在成为生物医学研究的前沿。作为精密医学研究的主要重点,癌症已被广泛接受为因遗传遗传变异或基因组损伤积累而引起的疾病。在单细胞水平上,用于癌症研究的微流控技术或芯片实验室技术是一种新兴工具,可用于改善风险评估,诊断类别和治疗策略。这项工作提出了一种用于单细胞基因表达谱分析的多层微芯片。用三种药物试剂(即甲磺酸甲酯,多西他赛和秋水仙碱)以不同的浓度和时间长度进行处理,然后将单个人乳腺癌细胞(MCF-7)裂解在芯片上,捕获释放的mRNA模板并将其反转录为cDNA。在微珠表面上。通过三重实时聚合酶链反应(qPCR)同时扩增和定量三个基因(GAPDH,CDKN1A,AURKA)。每次运行的读数设置为18,并且可以通过相同的方法进一步提高。该微芯片能够整合单细胞基因表达谱的所有步骤,并通过减少每个反应的试剂消耗和仪器成本来提供药物诱导的遗传毒性的精确研究。

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