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Defining the quantitative limits of intravital two-photon lymphocyte tracking

机译:确定体内双光子淋巴细胞跟踪的定量限

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Two-photon microscopy has substantially advanced our understanding of cellular dynamics in the immune system. Cell migration can now be imaged in real time in the living animal. Strikingly, the migration of naive lymphocytes in secondary lymphoid tissue appears predominantly random. It is unclear, however, whether directed migration may escape detection in this random background. Using a combination of mathematical modeling and experimental data, we investigate the extent to which modem two-photon imaging can rule out biologically relevant directed migration. For naive T cells migrating in uninfected lymph nodes (LNs) at average 3D speeds of around 18 nm/min, we rule out uniform directed migration of more than 1.7 pm/min at the 95% confidence level, confirming that T cell migration is indeed mostly random on a timescale of minutes. To investigate whether this finding still holds for longer timescales, we use a 3D simulation of the naive T cell LN transit. A pure random walk predicts a transit time of around 16 h, which is in good agreement with experimental results. A directional bias of only 0.5 μm/min—less than 3% of the cell speed—would already accelerate the transit twofold. These results jointly strengthen the random walk analogy for naive T cell migration in LNs, but they also emphasize that very small deviations from random migration can still be important Our methods are applicable to cells of any type and can be used to reanalyze existing datasets.
机译:双光子显微镜已大大提高了我们对免疫系统中细胞动力学的理解。现在可以在活体动物中实时成像细胞迁移。令人惊讶的是,幼稚淋巴细胞在次级淋巴组织中的迁移主要是随机的。但是,尚不清楚在这种随机背景下定向迁移是否可以逃避检测。使用数学建模和实验数据的组合,我们调查了现代双光子成像可以排除生物学相关的定向迁移的程度。对于未感染的T细胞以约18 nm / min的平均3D速度在未感染的淋巴结(LN)中迁移,我们排除了95%置信水平下超过1.7 pm / min的均匀定向迁移,这证实了T细胞的迁移确实是大部分时间都是随机的。为了调查这一发现是否仍然适用于更长的时间范围,我们使用了朴素的T细胞LN转运的3D模拟。纯随机游走预测的渡越时间约为16小时,这与实验结果非常吻合。仅0.5μm/ min的方向性偏差-不到电池速度的3%-就已经可以使传输加速两倍。这些结果共同加强了LN中朴素T细胞迁移的随机游走类比,但它们也强调与随机迁移的很小偏差仍然很重要。我们的方法适用于任何类型的细胞,可用于重新分析现有数据集。

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