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倾斜螺旋微流控技术用于超快速、无标记的循环肿瘤细胞分离。

Slanted spiral microfluidics for the ultra-fast, label-free isolation of circulating tumor cells.

机构信息

BioSystems and Micromechanics (BioSyM) IRG, Singapore-MIT Alliance for Research and Technology (SMART) Centre, Singapore.

出版信息

Lab Chip. 2014 Jan 7;14(1):128-37. doi: 10.1039/c3lc50617g.

Abstract

The enumeration and characterization of circulating tumor cells (CTCs), found in the peripheral blood of cancer patients, provide a potentially accessible source for cancer diagnosis and prognosis. This work reports on a novel spiral microfluidic device with a trapezoidal cross-section for ultra-fast, label-free enrichment of CTCs from clinically relevant blood volumes. The technique utilizes the inherent Dean vortex flows present in curvilinear microchannels under continuous flow, along with inertial lift forces which focus larger CTCs against the inner wall. Using a trapezoidal cross-section as opposed to a traditional rectangular cross-section, the position of the Dean vortex core can be altered to achieve separation. Smaller hematologic components are trapped in the Dean vortices skewed towards the outer channel walls and eventually removed at the outer outlet, while the larger CTCs equilibrate near the inner channel wall and are collected from the inner outlet. By using a single spiral microchannel with one inlet and two outlets, we have successfully isolated and recovered more than 80% of the tested cancer cell line cells (MCF-7, T24 and MDA-MB-231) spiked in 7.5 mL of blood within 8 min with extremely high purity (400-680 WBCs mL(-1); ~4 log depletion of WBCs). Putative CTCs were detected and isolated from 100% of the patient samples (n = 10) with advanced stage metastatic breast and lung cancer using standard biomarkers (CK, CD45 and DAPI) with the frequencies ranging from 3-125 CTCs mL(-1). We expect this simple and elegant approach can surmount the shortcomings of traditional affinity-based CTC isolation techniques as well as enable fundamental studies on CTCs to guide treatment and enhance patient care.

摘要

循环肿瘤细胞(CTC)的计数和特征,在癌症患者的外周血中发现,为癌症诊断和预后提供了一个潜在的可及来源。本工作报道了一种新颖的螺旋微流控装置,具有梯形横截面,可从临床相关的血液量中快速、无标记地富集 CTC。该技术利用在连续流动下曲线微通道中存在的固有迪恩涡旋流,以及惯性升力将较大的 CTC 聚焦到内壁。与传统的矩形横截面相比,使用梯形横截面可以改变迪恩涡核的位置以实现分离。较小的血液成分被困在偏向外通道壁的迪恩涡中,并最终在外出口处被去除,而较大的 CTC 则在靠近内通道壁的位置平衡,并从内出口收集。通过使用一个具有一个入口和两个出口的单个螺旋微通道,我们成功地在 8 分钟内从 7.5 毫升血液中分离和回收了超过 80%的测试癌细胞系细胞(MCF-7、T24 和 MDA-MB-231),纯度极高(400-680 WBCs mL(-1);白细胞减少 4 个对数级)。使用标准生物标志物(CK、CD45 和 DAPI)从 100%的晚期转移性乳腺癌和肺癌患者样本中检测和分离出了推定的 CTC,频率范围为 3-125 CTCs mL(-1)。我们期望这种简单而优雅的方法能够克服传统基于亲和力的 CTC 分离技术的缺点,并能够对 CTC 进行基础研究,以指导治疗和增强患者护理。

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