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首页> 外文期刊>International Journal of Cancer =: Journal International du Cancer >A novel (19)F agent for detection and quantification of human dendritic cells using magnetic resonance imaging.
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A novel (19)F agent for detection and quantification of human dendritic cells using magnetic resonance imaging.

机译:一种新型(19)F剂,用于使用磁共振成像检测和定量人类树突状细胞。

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Monitoring of cell therapeutics in vivo is of major importance to estimate its efficacy. Here, we present a novel intracellular label for (19)F magnetic resonance imaging (MRI)-based cell tracking, which allows for noninvasive, longitudinal cell tracking without the use of radioisotopes. A key advantage of (19)F MRI is that it allows for absolute quantification of cell numbers directly from the MRI data. The (19)F label was tested in primary human monocyte-derived dendritic cells. These cells took up label effectively, resulting in a labeling of 1.7 +/- 0.1 x 10(13) (19)F atoms per cell, with a viability of 80 +/- 6%, without the need for electroporation or transfection agents. This results in a minimum detection sensitivity of about 2,000 cells/voxel at 7 T, comparable with gadolinium-labeled cells. Comparison of the detection sensitivity of cells labeled with (19)F, iron oxide and gadolinium over typical tissue background showed that unambiguous detection of the (19)F-labeled cells was simpler than with the contrast agents. The effect of the (19)F agent on cell function was minimal in the context of cell-based vaccines. From these data, we calculate that detection of 30,000 cells in vivo at 3 T with a reasonable signal to noise ratio for (19)F images would require less than 30 min with a conventional fast spin echo sequence, given a coil similar to the one used in this study. This is well within acceptable limits for clinical studies, and thus, we conclude that (19)F MRI for quantitative cell tracking in a clinical setting has great potential.
机译:体内对细胞治疗剂的监测对于评估其疗效至关重要。在这里,我们提出了基于(19)F磁共振成像(MRI)的细胞跟踪的新型细胞内标签,它允许在不使用放射性同位素的情况下进行无创纵向细胞跟踪。 (19)F MRI的主要优势在于,它可以直接从MRI数据中对细胞数进行绝对定量。在原代人单核细胞衍生的树突状细胞中测试了(19)F标签。这些细胞有效地吸收了标记,导致每个细胞标记1.7 +/- 0.1 x 10(13)(19)F原子,存活力为80 +/- 6%,而无需电穿孔或转染试剂。这导致在7 T时的最小检测灵敏度约为2,000个细胞/体素,与g标记的细胞相当。比较在典型组织背景下用(19)F,氧化铁和g标记的细胞的检测灵敏度,发现(19)F标记的细胞的明确检测比使用造影剂更简单。在基于细胞的疫苗中,(19)F剂对细胞功能的影响极小。根据这些数据,我们计算出,对于常规的快速自旋回波序列,如果以合理的信噪比对(19)F图像进行3 T检测,在3 T下检测到30,000个细胞将需要不到30分钟的时间,并且线圈类似于一个在这项研究中使用。这完全在临床研究可接受的范围内,因此,我们得出结论:(19)F MRI在临床环境中用于定量细胞追踪具有巨大的潜力。

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