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实时变形细胞术揭示中性粒细胞致敏过程中的顺序收缩和扩张。

Real-time deformability cytometry reveals sequential contraction and expansion during neutrophil priming.

机构信息

Department of Medicine, University of Cambridge, Cambridge, UK.

National Institutes of Health, Bethesda, Maryland, USA.

出版信息

J Leukoc Biol. 2019 Jun;105(6):1143-1153. doi: 10.1002/JLB.MA0718-295RR. Epub 2019 Mar 5.

Abstract

It has become increasingly apparent that the biomechanical properties of neutrophils impact on their trafficking through the circulation and in particularly through the pulmonary capillary bed. The retention of polarized or shape-changed neutrophils in the lungs was recently proposed to contribute to acute respiratory distress syndrome pathogenesis. Accordingly, this study tested the hypothesis that neutrophil priming is coupled to morpho-rheological (MORE) changes capable of altering cell function. We employ real-time deformability cytometry (RT-DC), a recently developed, rapid, and sensitive way to assess the distribution of size, shape, and deformability of thousands of cells within seconds. During RT-DC analysis, neutrophils can be easily identified within anticoagulated "whole blood" due to their unique granularity and size, thus avoiding the need for further isolation techniques, which affect biomechanical cell properties. Hence, RT-DC is uniquely suited to describe the kinetics of MORE cell changes. We reveal that, following activation or priming, neutrophils undergo a short period of cell shrinking and stiffening, followed by a phase of cell expansion and softening. In some contexts, neutrophils ultimately recover their un-primed mechanical phenotype. The mechanism(s) underlying changes in human neutrophil size are shown to be Na /H antiport-dependent and are predicted to have profound implications for neutrophil movement through the vascular system in health and disease.

摘要

越来越明显的是,中性粒细胞的生物力学特性会影响其在血液循环中的迁移,特别是在穿过肺毛细血管床时。最近有人提出,极化或形态改变的中性粒细胞在肺部的滞留可能有助于急性呼吸窘迫综合征的发病机制。因此,本研究检验了这样一个假设,即中性粒细胞的激活与形态流变学(MORE)变化有关,这些变化能够改变细胞功能。我们采用实时变形细胞术(RT-DC),这是一种最近开发的快速、敏感的方法,可以在几秒钟内评估数千个细胞的大小、形状和变形性分布。在 RT-DC 分析中,由于中性粒细胞独特的颗粒度和大小,它们可以很容易地在抗凝“全血”中被识别出来,从而避免了进一步的分离技术,这些技术会影响生物力学细胞特性。因此,RT-DC 非常适合描述 MORE 细胞变化的动力学。我们发现,中性粒细胞在激活或激活后会经历短暂的细胞收缩和变硬阶段,然后是细胞扩张和变软阶段。在某些情况下,中性粒细胞最终会恢复其未激活的机械表型。人类中性粒细胞大小变化的机制被证明是 Na+/H 反向转运依赖的,并可能对中性粒细胞在健康和疾病状态下通过血管系统的迁移产生深远影响。

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