Literature DB >> 2327657

Neutrophil kinetics in the pulmonary microcirculation. Effects of pressure and flow in the dependent lung.

D C Lien1, G S Worthen, R L Capen, W L Hanson, L L Checkley, S J Janke, P M Henson, W W Wagner.   

Abstract

Increases in pulmonary arterial pressure or blood flow raise peripheral white cell count by releasing sequestered leukocytes from the lung. The effects of altered hemodynamics, however, on the leukocyte sequestration site and on the distribution of leukocyte transit times through the pulmonary microcirculation are unknown. We used in vivo fluorescence videomicroscopy to study the passage of individual, fluorescein-isothiocyanate-labeled neutrophils through the pulmonary microcirculation of anesthetized dogs. Pulmonary hemodynamics were altered over a wide range. Regardless of the hemodynamic conditions, the only place that any of the 2,919 observed neutrophils stopped was in the capillaries. The periods of immobility had a wide range, from less than 1 to greater than 1,200 s. Because the cells remained motionless once they stopped and then accelerated suddenly as they regained the free-flowing stream, the obstructions must have been discrete. About a quarter of the capillary pathways had one site of high resistance. Another quarter offered two or more obstructions. In the remaining half, the neutrophils passed rapidly and without pause from arteriole to venule. Increases in pressure and flow decreased the number of times that individual cells stopped. These changes altered the median transit time by shifting the distribution of transit times between the slowest and fastest groups. We conclude that most of the total pathlength of perfused capillaries offers little resistance even to neutrophils. There are, however, focal areas in individual capillaries that offer high resistance to neutrophil passage.

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Year:  1990        PMID: 2327657     DOI: 10.1164/ajrccm/141.4_Pt_1.953

Source DB:  PubMed          Journal:  Am Rev Respir Dis        ISSN: 0003-0805


  8 in total

1.  Neutrophil transit times through pulmonary capillaries: the effects of capillary geometry and fMLP-stimulation.

Authors:  Mark Bathe; Atsushi Shirai; Claire M Doerschuk; Roger D Kamm
Journal:  Biophys J       Date:  2002-10       Impact factor: 4.033

Review 2.  New perspectives on basic mechanisms in lung disease. 2. Neutrophil traffic in the lungs: role of haemodynamics, cell adhesion, and deformability.

Authors:  W MacNee; C Selby
Journal:  Thorax       Date:  1993-01       Impact factor: 9.139

3.  Neutrophil cytoskeletal rearrangements during capillary sequestration in bacterial pneumonia in rats.

Authors:  Kazuo Yoshida; Ryoichi Kondo; Qin Wang; Claire M Doerschuk
Journal:  Am J Respir Crit Care Med       Date:  2006-06-01       Impact factor: 21.405

4.  Quantitative Pulmonary Neutrophil Dynamics Using Computer-Vision Stabilized Intravital Imaging.

Authors:  Yoshikazu Tsukasaki; Peter T Toth; Esmaeil Davoodi-Bojd; Jalees Rehman; Asrar B Malik
Journal:  Am J Respir Cell Mol Biol       Date:  2022-01       Impact factor: 7.748

5.  A murine model to study leukocyte rolling and intravascular trafficking in lung microvessels.

Authors:  Lyudmila Sikora; Asa C M Johansson; Savita P Rao; Greg K Hughes; David H Broide; P Sriramarao
Journal:  Am J Pathol       Date:  2003-06       Impact factor: 4.307

6.  Threshold size for optimal passive pulmonary targeting and retention of rigid microparticles in rats.

Authors:  Hilliard L Kutscher; Piyun Chao; Manjeet Deshmukh; Yashveer Singh; Peidi Hu; Laurie B Joseph; David C Reimer; Stanley Stein; Debra L Laskin; Patrick J Sinko
Journal:  J Control Release       Date:  2010-01-05       Impact factor: 9.776

7.  Neutrophil sequestration in rat lungs.

Authors:  G M Brown; D M Brown; K Donaldson; E Drost; W MacNee
Journal:  Thorax       Date:  1995-06       Impact factor: 9.139

Review 8.  Biomechanics of the Circulating Tumor Cell Microenvironment.

Authors:  Benjamin L Krog; Michael D Henry
Journal:  Adv Exp Med Biol       Date:  2018       Impact factor: 2.622

  8 in total

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