Molecular Mechanisms of Monocyte Adhesion to Interleukin-1β–Stimulated Endothelial Cells Under Physiologic Flow Conditions

Author:

Kukreti Sharad1,Konstantopoulos Konstantinos1,Smith C. Wayne1,McIntire Larry V.1

Affiliation:

1. From the Cox Laboratory for Biomedical Engineering, Rice University, and Speros P. Martel Laboratory of Leukocyte Biology, Departments of Pediatrics and Microbiology & Immunology, Baylor College of Medicine, Houston, TX.

Abstract

Abstract This study identifies multiple pathways used by monocytes to adhere to 4-hour interleukin-1β stimulated human umbilical vein endothelial cells under flow conditions. Physiologic shear stresses were simulated in a flow chamber with parallel plate geometry; quantitation of primary adhesion, secondary adhesion, and transmigration was performed using phase contrast videomicroscopy. Neuraminidase treatment of monocytes reduced primary interaction by 50%, whereas blocking L-selectin or very late antigen-4 showed significant but smaller effects (∼30% inhibition). However, a combined treatment against all three pathways was able to reduce interaction by 80%. Blocking β2 and α4 integrin pathways together inhibited secondary/firm adhesion by 75%. Only 40% of firmly adherent monocytes transmigrated across the endothelial monolayer with significantly increased transmigration times when both β2 and α4 integrins were blocked. These results demonstrate that monocytes can use multiple receptors to interact with endothelial cells at both primary and secondary adhesion stages, and that these pathways have to be blocked simultaneously for maximum inhibition.

Publisher

American Society of Hematology

Subject

Cell Biology,Hematology,Immunology,Biochemistry

Reference31 articles.

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5. Monocyte rolling, arrest and spreading on IL-4 activated vascular endothelium under flow is mediated via sequential action of L-selectin, β1 -integrins, and β2 -integrins.;Luscinskas;J Cell Biol,1994

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