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COMPOUND DROPLET MODELLING OF CIRCULATING TUMOR CELL MICROFILTRATION

机译:循环肿瘤细胞微滤的复合液滴模型

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The Circulating Tumor Cell (CTC) is the cancer cell that has shed into the circulation system (i.e. cancer cell in the bloodstream). These CTCs are potential indicators for early cancer detection, which is critical for the whole process in cancer treatment. Among all new techniques, early detection of cancer from a single blood drop sample using the mechanical method by CTC microfiltration is promising for its simplicity, low cost, and ease of use. In the microfiltration of circulating tumor cells, the problem of a single CTC passing through a microfilter at a constant flow rate is a basic model for further device design and optimization. In our present paper, we developed a compound droplet model for the CTC passing through a microfilter. Numerically, we used the Volume of Fraction (VOF), three phase flow method. In this model, we take the blood, CTC cytoplasm and CTC nucleus as three individual fluids/phases. To build a more realistic model, the CTC cytoplasm and nucleus are taken as two fluids with their own surface tension coefficients and viscosities; the viscosity of the cytoplasm is considered as twice that of the bloodstream; the stiffness of the nucleus is set as four times that of the cytoplasm. Through the pressure signature and CTC deformation, the interaction between the compound droplet CTC, bloodstream, as well as the channel wall are studied numerically. As demonstrated in the previous Newtonian single droplet model, this critical passing pressure can be predicted by Young-Laplace equation. However, for the compound droplet model, no equation description is available. Through our study, the critical passing pressure, as well as the dynamic process of CTC passing pressure signature, is provided together with corresponding CTC deformation in each key stage. The pressure signature and deformation difference between the simple droplet model and compound droplet model are also compared. Additionally, the biological parameter, like the radius of cancer nucleus, is also an important parameter in the early cancer detection device design. In the following part of our study, we introduced a clinical parameter called N/C ratio, or nucleus/ cytoplasm ratio, which is a key parameter to discriminate between the healthy cell and tumor cell. By bringing this parameter into our study, the interaction among the nucleus, cytoplasm, bloodstream, as well as the wall of microfilter are studied for soft, medium and hard CTCs. In the end, the drawback of our method is also provided with advice for improvement.
机译:循环肿瘤细胞(CTC)是癌细胞,其落入循环系统(即血液中的癌细胞)。这些CTC是早期癌症检测的潜在指标,这对于癌症治疗的整个过程至关重要。在所有新技术中,通过CTC微滤的机械方法从单血滴样品早期检测癌症的早期检测是其简单性,低成本和易用性的希望。在循环肿瘤细胞的微滤中,通过以恒定流速通过微过滤器的单个CTC的问题是进一步的装置设计和优化的基本模型。在我们现在的论文中,我们开发了一种用于通过微过滤器的CTC的复合液滴模型。在数值上,我们使用了分数(VOF)的体积,三相流法。在该模型中,我们将血液,CTC细胞质和CTC核作为三个单独的流体/相。为了构建更现实的模型,CTC细胞质和核被用作其表面张力系数和粘度的两个流体;细胞质的粘度被认为是血液的两倍;细胞核的刚度设定为细胞质的四倍。通过压力签名和CTC变形,在数值上研究了复合液滴CTC,血液以及通道壁之间的相互作用。如在以前的牛顿单液滴模型中所示,杨拉普拉斯方程可以预测这种关键的通过压力。然而,对于复合液滴模型,没有公式描述。通过我们的研究,临界通过压力以及CTC通过压力签名的动态过程,在每个键阶段中与相应的CTC变形一起提供。还比较了简单液滴模型和复合液滴模型之间的压力特征和变形差异。另外,生物学参数,如癌症核的半径,也是早期癌症检测装置设计中的重要参数。在我们研究的以下部分中,我们介绍了一种名为N / C比的临床参数,或核/细胞质比,这是区分健康细胞和肿瘤细胞之间的关键参数。通过将该参数置于我们的研究中,研究了核,细胞质,血液的相互作用以及微过滤器的壁,用于软,中和硬质CTC。最后,还提供了我们方法的缺点,提出了改进的建议。

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