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The ART mu S: a novel microfluidic CD4+T-cell enumeration system for monitoring antiretroviral therapy in HIV patients

机译:ARTμS:一种新型的微流控CD4 + T细胞计数系统,用于监测HIV患者的抗逆转录病毒疗法

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摘要

We report on a novel and cost-effective microfluidic platform that integrates immunomagnetic separation and cell enumeration via DNA-induced bead aggregation. Using a two-stage immunocapture microdevice, 10 mu L of whole blood was processed to isolate CD4+ T-cells. The first stage involved the immuno-subtraction of monocytes by anti-CD14 magnetic beads, followed by CD4+ T-cell capture with anti-CD4 magnetic beads. The super hydrophilic surface generated during polydimethylsiloxane (PDMS) plasma treatment allowed for accurate metering of the CD4+ T-cell lysate, which then interacted with silica-coated magnetic beads under chaotropic conditions to form aggregates. Images of the resulting aggregates were captured and processed to reveal the mass of DNA, which was used to back-calculate the CD4+ T-cell number. Studies with clinical samples revealed that the analysis of blood within 24 hours of phlebotomy yielded the best results. Under these conditions, an accurate cell count was achieved (R-2 = 0.98) when compared to cell enumeration via flow cytometry, and over a functional dynamic range from 106-2337 cells per mu L.
机译:我们报告了一个新颖的,具有成本效益的微流控平台,整合了免疫磁分离和通过DNA诱导的珠子聚集的细胞计数。使用两阶段免疫捕获微设备,处理10μL全血以分离CD4 + T细胞。第一阶段涉及通过抗CD14磁珠对单核细胞进行免疫减法,然后用抗CD4磁珠捕获CD4 + T细胞。在聚二甲基硅氧烷(PDMS)等离子体处理过程中产生的超亲水表面可以精确计量CD4 + T细胞裂解物,然后在离液条件下与二氧化硅包覆的磁珠相互作用,形成聚集体。捕获并处理所得聚集体的图像,以揭示DNA的质量,该质量用于反算CD4 + T细胞数。对临床样品的研究表明,放血24小时内对血液的分析产生了最佳结果。在这些条件下,与通过流式细胞仪进行的细胞计数相比,可以实现准确的细胞计数(R-2 = 0.98),并且功能动态范围为每μL 106-2337个细胞。

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