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首页> 外文期刊>International Journal of Nanomedicine >Quantitative detection of the tumor-associated antigen large external antigen in colorectal cancer tissues and cells using quantum dot probe
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Quantitative detection of the tumor-associated antigen large external antigen in colorectal cancer tissues and cells using quantum dot probe

机译:量子点探针定量检测大肠癌组织和细胞中肿瘤相关抗原大外部抗原

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The large external antigen (LEA) is a cell surface glycoprotein that has been proven to be highly expressed in colorectal cancer (CRC) as a tumor-associated antigen. To?evaluate and validate the relationship between LEA expression and clinical characteristics of CRC with high efficiency, LEA expression levels were detected in 85 tissue blocks from CRC patients by quantum dot-based immunohistochemistry (QD-IHC) combined with imaging quantitative analysis using quantum dots with a 605 nm emission wavelength (QD605) conjugated to an ND-1 monoclonal antibody against LEA as a probe. Conventional IHC was performed in parallel for comparison. Both QD-IHC and conventional IHC showed that LEA was specifically expressed in CRC, but not in non-CRC tissues, and high LEA expression was significantly associated with a more advanced T-stage ( P <0.05), indicating that LEA is likely to serve as a CRC prognostic marker. Compared with conventional IHC, receiver operating characteristic analysis revealed that QD-IHC possessed higher sensitivity, resulting in an increased positive detection rate of CRC, from 70.1% to 89.6%. In addition, a simpler operation, objective analysis of results, and excellent repeatability make QD-IHC an attractive alternative to conventional IHC in clinical practice. Furthermore, to explore whether the QD probes can be utilized to quantitatively detect living cells or single cells, quantum dot-based immunocytochemistry (QD-ICC) combined with imaging quantitative analysis was developed to evaluate LEA expression in several CRC cell lines. It was demonstrated that QD-ICC could also predict the correlation between LEA expression and the T-stage characteristics of the cell lines, which was confirmed by flow cytometry. The results of this study indicate that QD-ICC has the potential to noninvasively detect rare circulating tumor cells in clinical samples in real clinical applications.
机译:大的外部抗原(LEA)是一种细胞表面糖蛋白,已被证明在大肠癌(CRC)中作为肿瘤相关抗原高表达。为了高效地评估和验证LEA表达与CRC临床特征之间的关系,通过基于量子点的免疫组织化学(QD-IHC)结合量子点成像定量分析在CRC患者的85个组织块中检测到LEA表达水平与605 nm发射波长(QD605)偶联的抗LEA ND-1单克隆抗体作为探针。并行进行常规IHC进行比较。 QD-IHC和常规IHC均显示LEA在CRC中特异性表达,但在非CRC组织中不表达,并且LEA高表达与更晚期的T期显着相关(P <0.05),表明LEA可能用作CRC预后指标。与常规IHC相比,接收机工作特性分析显示QD-IHC具有更高的灵敏度,从而使CRC的阳性检出率从70.1%提高到89.6%。此外,更简单的操作,对结果的客观分析以及出色的可重复性使QD-IHC在临床实践中成为常规IHC的有吸引力的替代品。此外,为了探索QD探针是否可用于定量检测活细胞或单细胞,开发了基于量子点的免疫细胞化学(QD-ICC)与成像定量分析相结合的方法,以评估LEA在几种CRC细胞系中的表达。通过流式细胞术证实,QD-ICC还可以预测LEA表达与细胞系T期特征之间的相关性。这项研究的结果表明,QD-ICC具有在实际临床应用中无创检测临床样品中稀有循环肿瘤细胞的潜力。

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