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The architecture of neutrophil extracellular traps investigated by atomic force microscopy

机译:中性粒细胞胞外结构的陷阱通过原子力显微镜研究了

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Neutrophils are immune cells that engage in a suicidal pathway leading to the release of partially decondensed chromatin, or neutrophil extracellular traps (NETs). NETs behave as a double edged sword; they can bind to pathogens thereby ensnaring them and limiting their spread during infection; however, they may bind to host circulating materials and trigger thrombotic events, and are associated with autoimmune disorders. Despite the fundamental role of NETs as part of an immune system response, there is currently a very poor understanding of how their nanoscale properties are reflected in their macroscopic impact. In this work, using a combination of fluorescence and atomic force microscopy, we show that NETs appear as a branching filament network that results in a substantially organized porous structure with openings with 0.03 +/- 0.04 mu m(2) on average and thus in the size range of small pathogens. Topological profiles typically up to 3 +/- 1 nm in height are compatible with a "beads on a string" model of nucleosome chromatin. Typical branch lengths of 153 +/- 103 nm appearing as rigid rods and height profiles of naked DNA in NETs of 1.2 +/- 0.5 nm are indicative of extensive DNA supercoiling throughout NETs. The presence of DNA duplexes could also be inferred from force spectroscopy and the occurrence of force plateaus that ranged from similar to 65 pN to 300 pN. Proteolytic digestion of NETs resulted in widespread disassembly of the network structure and considerable loss of mechanical properties. Our results suggest that the underlying structure of NETs is considerably organized and that part of its protein content plays an important role in maintaining its mesh architecture. We anticipate that NETs may work as microscopic mechanical sieves with elastic properties that stem from their DNA-protein composition, which is able to segregate particles also as a result of their size. Such a behavior may explain their participation in capturing pathogens and their association with thrombosis.
机译:中性粒细胞是参与的免疫细胞自杀的途径导致的释放部分decondensed染色质,或嗜中性粒细胞细胞外陷阱(网)。双刃的剑;从而牵扯了他们,限制他们的传播在感染;循环材料和引发血栓性事件,与自身免疫有关障碍。作为免疫系统反应的一部分,有目前一个非常贫穷的了解他们反映在他们的纳米级属性宏观的影响。结合荧光和原子力显微镜,我们表明,网作为一个出现在一个分支长丝网络,结果有序多孔结构开口和0.03 + / - 0.04μm(2)平均因此小尺寸范围的病原体。拓扑配置文件通常3 + / - 1海里在高度兼容“珠子字符串“核小体染色质的典范。分支长度的153 + / - 103海里出现刚性杆和高度的裸DNA网的1.2 + / - 0.5 nm的象征在网广泛成为超螺旋DNA。存在的DNA工器也可以推断从光谱和发生高原,范围从类似于65年pN力量300 pN。在广泛的网络的拆卸结构和机械的巨大损失属性。网的底层结构组织,其蛋白质含量的一部分在保持其网中扮演一个重要的角色体系结构。微观力学与弹性筛子属性,源于他们的dna蛋白质成分,能够隔离粒子也由于他们的尺寸。可以解释他们的参与捕捉吗病原体及其与血栓形成有关。

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