ICAM-2, JAM-A, and PECAM-1 mediate leukocyte transmigration in vivo in C57BL/6 mice in a stimulus-dependent manner
| Junctional protein . | Dependent . | Independent . |
|---|---|---|
| ICAM-2 | IL-1β,14 ischemia/reperfusion injury* | TNF-α,14 thioglycollate,14 LTB4* |
| JAM-A | IL-1β,8 ischemia/reperfusion injury8 | LTB4,8 PAF8 |
| PECAM-1 | IL-1β15 | TNF-α,15 thioglycollate22 |
| Junctional protein . | Dependent . | Independent . |
|---|---|---|
| ICAM-2 | IL-1β,14 ischemia/reperfusion injury* | TNF-α,14 thioglycollate,14 LTB4* |
| JAM-A | IL-1β,8 ischemia/reperfusion injury8 | LTB4,8 PAF8 |
| PECAM-1 | IL-1β15 | TNF-α,15 thioglycollate22 |
The table summarizes previous data from our group showing that the ability of the endothelial cell junctional molecules ICAM-2, JAM-A, and PECAM-1 to mediate leukocyte transmigration is dependent on the nature of the stimulus. All these studies were conducted in C57BL/6 mice.
Unpublished data.