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Two-dimensional kinetics of β2-integrin and ICAM-1 bindings between neutrophils and melanoma cells in a shear flow

机译:剪切流中嗜中性粒细胞和黑色素瘤细胞之间β2-整合素和ICAM-1结合的二维动力学

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摘要

Cell adhesion, mediated by specific receptor-ligand interactions, plays an important role in biological processes such as tumor metastasis and inflammatory cascade. For example, interactions between β2-integrin (lymphocyte function-associated antigen-1 and/or Mac-1) on polymorphonuclear neutrophils (PMNs) and ICAM-1 on melanoma cells initiate the bindings of melanoma cells to PMNs within the tumor microenvironment in blood flow, which in turn activate PMN-melanoma cell aggregation in a near-wall region of the vascular endothelium, therefore enhancing subsequent extravasation of melanoma cells in the microcirculations. Kinetics of integrin-ligand bindings in a shear flow is the determinant of such a process, which has not been well understood. In the present study, interactions of PMNs with WM9 melanoma cells were investigated to quantify the kinetics of β2-integrin and ICAM-1 bindings using a cone-plate viscometer that generates a linear shear flow combined with a two-color flow cytometry technique. Aggregation fractions exhibited a transition phase where it first increased before 60 s and then decreased with shear durations. Melanoma-PMN aggregation was also found to be inversely correlated with the shear rate. A previously developed probabilistic model was modified to predict the time dependence of aggregation fractions at different shear rates and medium viscosities. Kinetic parameters of β2-integrin and ICAM-1 bindings were obtained by individual or global fittings, which were comparable to respectively published values. These findings provide new quantitative understanding of the biophysical basis of leukocyte-tumor cell interactions mediated by specific receptor-ligand interactions under shear flow conditions.
机译:由特异性受体-配体相互作用介导的细胞粘附在生物学过程如肿瘤转移和炎症级联中起重要作用。例如,多形核中性粒细胞(PMN)上的β2-整合素(淋巴细胞功能相关抗原-1和/或Mac-1)与黑色素瘤细胞上的ICAM-1之间的相互作用启动了黑色素瘤细胞与血液中肿瘤微环境内的PMN的结合流动,继而激活血管内皮近壁区域中的PMN-黑素瘤细胞聚集,因此增强了微循环中黑素瘤细胞的随后外渗。剪切流中整联蛋白-配体结合的动力学是这种过程的决定因素,目前尚不清楚。在本研究中,使用锥板粘度计产生线性剪切流并结合双色流式细胞仪,研究了PMN与WM9黑色素瘤细胞之间的相互作用,以量化β2-整联蛋白和ICAM-1结合的动力学。聚集分数表现出一个过渡阶段,在过渡阶段,它首先在60 s之前增加,然后随剪切持续时间而减少。还发现黑素瘤-PMN聚集与剪切速率成反比。修改了以前开发的概率模型,以预测在不同剪切速率和中等粘度下聚集分数的时间依赖性。 β2-整联蛋白和ICAM-1结合的动力学参数是通过单独或整体拟合获得的,可与分别发表的值相比较。这些发现为在剪切流条件下由特定受体-配体相互作用介导的白细胞-肿瘤细胞相互作用的生物物理基础提供了新的定量理解。

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