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首页> 外文期刊>Mutation research-Fundamental and Molecular Mechanisms of Mutagenesis >Simultaneous detection of tumor markers in lung cancer using scanning electrochemical microscopy
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Simultaneous detection of tumor markers in lung cancer using scanning electrochemical microscopy

机译:扫描电化学显微镜同时检测肺癌肿瘤标志物

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摘要

Cancer became a global public health problem and one of the most causes of death, and early diagnosis will decrease mortality and extend lifespan of patients. In this study, the simultaneous detection of four tumor markers in lung cancer (alpha-fetoprotein (AFP), carcinoembryonic antigen (CEA), neuron-specific enolase (NSE), cytokeratin-19-fragment (Cyfra21-1)) was achieved for the first time using immune sandwich structures coupled with generation collection (GC) mode of scanning electrochemical microscopy (SECM). The proposed method exhibited excellent performance in quantitative detection of the four target proteins. A good linear correlation between the signal current issued from reduction of p-benzoquinone (BQ) oxidized from hydroquinone (H(2)Q) and the amount of target tumor markers at logarithmic protein concentrations ranging from 5 ng/mL to 1 mu g/mL was achieved. The detection limit was also low, meeting the needs of clinical use. The specificity was satisfactory and signal current of the target protein was unaffected by other simultaneously detected target proteins and common interfering species. Overall, the proposed method looks promising for high-throughput protein determination based on SECM, which could potentially be applied in clinical lung cancer diagnosis.
机译:癌症成为全球性的公共卫生问题,最多的死亡原因之一,早期诊断将降低死亡率并延长患者的寿命。在本研究中,实现了肺癌中四种肿瘤标志物(α-胎儿(AHα-胎蛋白(AFP),癌症胺抗原(CEA),神经元特异性烯醇酶(NSE),细胞角蛋白-19-片段(CYFRA21-1)中的四种肿瘤标志物。第一次使用免疫夹层结构与扫描电化学显微镜(SECM)的产生收集(GC)模式耦合。该方法在四个靶蛋白的定量检测中表现出优异的性能。从氢醌(H(2)Q)氧化的低苯醌(BQ)减少的信号电流之间的良好线性相关性和对数蛋白浓度的靶肿瘤标志物的量,范围为5 ng / ml至1μg/实现ml。检测极限也很低,满足临床使用的需要。特异性是令人满意的,并且目标蛋白的信号电流不受其他同时检测到的靶蛋白和常见干扰物种的影响。总体而言,该方法看起来对基于SECM的高通量蛋白质测定,这可能适用于临床肺癌诊断。

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