Paradoxical attenuation of leukocyte rolling in response to ischemia- reperfusion and extracorporeal blood circulation in inflamed tissue.

6533b7d7fe1ef96bd1267ad0

RESEARCH PRODUCT

Paradoxical attenuation of leukocyte rolling in response to ischemia- reperfusion and extracorporeal blood circulation in inflamed tissue.

Desiree N. Sehrt Markus Kamler Heinz Jakob Hans-anton Lehr Stephan C. Schäfer

subject

medicine.medical_specialty Extracorporeal Circulation Physiology Ischemia Leukocyte Rolling Leukotriene B4 Extracorporeal Microcirculation Venules Physiology (medical)Internal medicine Cricetinae Medicine Animals Leukocyte Rolling Muscle Skeletal Mesocricetus Myositis business.industry Extracorporeal circulation Anatomy medicine.disease Microscopy Fluorescence Reperfusion Injury Cremaster muscle Circulatory system Cardiology Cardiology and Cardiovascular Medicine business Reperfusion injury

description

In contrast to acute preparations such as the exteriorized mesentery or the cremaster muscle, chronically instrumented chamber models allow one to study the microcirculation under “physiological” conditions, i.e., in the absence of trauma-induced leukocyte rolling along the venular endothelium. To underscore the importance of studying the naive microcirculation, we implanted titanium dorsal skinfold chambers in hamsters and used intravital fluorescence microscopy to study venular leukocyte rolling in response to ischemia-reperfusion injury or extracorporeal blood circulation. The experiments were performed in chambers that fulfilled all well-established criteria for a physiological microcirculation as well as in chambers that showed various extents of leukocyte rolling due to trauma, hemorrhage, or inflammation. In ideal chambers with a physiological microcirculation (<30 rolling leukocytes/mm vessel circumference in 30 s), ischemia-reperfusion injury and extracorporeal blood circulation significantly stimulated leukocyte rolling along the venular endothelium and, subsequently, firm leukocyte adhesion. In contrast, both stimuli failed to elicit leukocyte rolling in borderline chambers (30–100 leukocytes/mm), and in blatantly inflamed chambers with yet higher numbers of rolling leukocytes at baseline (>100 leukocytes/mm), we observed a paradoxical reduction of leukocyte rolling after ischemia-reperfusion injury or extracorporeal blood circulation. A similar effect was observed when we superfused leukotriene B4(LTB4) onto the chamber tissue. The initial increase in leukocyte rolling in response to an LTB4challenge was reversed by a second superfusion 90 min later. These observations underscore 1) the benefit of studying leukocyte-endothelial cell interaction in chronically instrumented chamber models and 2) the necessity to strictly adhere to well-established criteria of a physiological microcirculation.

year	journal	country	edition	language
2005-06-18	American journal of physiology. Heart and circulatory physiology

10.1152/ajpheart.00674.2004 https://pubmed.ncbi.nlm.nih.gov/15961377