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急性炎症期间肺微循环中的中性粒细胞动力学

Neutrophil kinetics in the pulmonary microcirculation during acute inflammation.

作者信息

Lien D C, Henson P M, Capen R L, Henson J E, Hanson W L, Wagner W W, Worthen G S

机构信息

Department of Pediatrics National Jewish Center for Immunology and Respiratory Medicine, Denver, Colorado.

出版信息

Lab Invest. 1991 Aug;65(2):145-59.

PMID:1908922
Abstract

The site of neutrophil interaction with the vasculature during acute lung inflammation is controversial, but has been suggested to occur in the alveolar capillaries, in contrast with its location in postcapillary venules in nonpulmonary tissues. We studied the kinetics of neutrophil accumulation and the site of neutrophil-vascular interaction in the lung by examining directly the behavior of fluorescein isothiocyanate-labeled canine neutrophils utilizing in vivo fluorescence videomicroscopy through a window inserted into the chest wall of anesthetized dogs. The administration of fragments of the fifth component of complement (C5f) into either the airway or pulmonary artery resulted in neutrophil sequestration almost exclusively in pulmonary capillaries. Kinetically, there was a shift in the distribution of neutrophil transit times resulting in a marked prolongation of median transit time. This response occurred within seconds after intravascular C5f and within 5 minutes after airway C5f and was maintained for at least 30 minutes. Ultrastructural studies after airway C5f showed neutrophils in various stages of migration through the alveolar-capillary membrane and more than 90% of these neutrophils were seen to migrate from capillary rather than from venular sites. These data indicate that pulmonary inflammation differs from inflammation in other vascular beds primarily in the site of neutrophil localization and migration. This fundamental difference in the inflammatory response may serve to localize the inflammatory response to the alveolus, and (since cells were retained singly), indicates the inability of leukoaggregation adequately to explain the findings. Leukocyte accumulation in the lung may thus occur through alterations in the balance between delivery of neutrophils to the lung and the transit time of these cells across the capillary bed.

摘要

在急性肺部炎症期间,中性粒细胞与脉管系统相互作用的部位存在争议,但有人提出这种相互作用发生在肺泡毛细血管中,这与它在非肺部组织的毛细血管后微静脉中的位置形成对比。我们通过利用体内荧光视频显微镜,直接观察异硫氰酸荧光素标记的犬中性粒细胞在麻醉犬胸壁插入窗口后的行为,研究了肺部中性粒细胞聚集的动力学以及中性粒细胞与血管相互作用的部位。将补体第五成分(C5f)片段注入气道或肺动脉后,中性粒细胞几乎完全滞留于肺毛细血管中。从动力学角度来看,中性粒细胞通过时间的分布发生了变化,导致中位通过时间显著延长。这种反应在血管内注入C5f后数秒内出现,在气道注入C5f后5分钟内出现,并持续至少30分钟。气道注入C5f后的超微结构研究显示,中性粒细胞处于穿过肺泡 - 毛细血管膜的不同迁移阶段,并且超过90%的这些中性粒细胞被观察到是从毛细血管而非微静脉部位迁移而来。这些数据表明,肺部炎症与其他血管床炎症的主要区别在于中性粒细胞定位和迁移的部位。炎症反应中的这种根本差异可能有助于将炎症反应局限于肺泡,并且(由于细胞是单个滞留的)表明白细胞聚集不足以充分解释这些发现。因此,肺部白细胞的聚集可能是通过中性粒细胞输送到肺部与这些细胞穿过毛细血管床的通过时间之间平衡的改变而发生的。

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