Focal effects of mononuclear leukocyte transendothelial migration: TNF-alpha production by migrating monocytes promotes subsequent migration of lymphocytes.

1996 
In many inflammatory diseases, mononu- clear leukocytes (MNLs) accumulate as focal infil- trates in perivascular spaces. We postulated that MNLS migrating through endothelium modify the microenvironment to promote the subsequent migra- tion of additional MNLS into the same area. We found that as monocytes adhere to and migrate spontane- ously through an endothelial monolayer, they secrete tumor necrosis factor-a (TNF-a) and interleukin- 1. These cytokines stimulate endothelial cell expression of CD54 (intercellular adhesion molecule-b) and CD1O6 (vascular cell adhesion molecule-b). Conse- quently, when freshly isolated MNLs are added to that endothelial monolayer four or more hours later, significantly greater numbers of lymphocytes bind to and migrate through these endothelial monolayers. In addition to its ability to activate endothelial cell adhesion molecules, TNF-a induced directed migra- tion of lymphocytes through collagen pads. These results illustrate a potential amplification mechanism by which MNLS moving through a vessel wall may secrete TNF-a, leading to the recruitment of addi- tional leukocytes into the same perivascular locus. J. Leukoc. Rio!. 60: 129-136; 1996.
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