Heparin attenuates TNF-á induced inflammatory response through a CD11b dependent mechanism

Background—In addition to its anticoagulant properties, heparin has antiinflammatory eVects, the molecular and mechanistic bases of which are incompletely defined. Aims—The current studies were designed to test the hypothesis that heparin abrogates the expression or function of leucocyte-endothelial adherence molecules which are fundamental to the acute inflammatory response. Methods—The eVects of heparin on tumour necrosis factor alpha (TNF-á) induced leucocyte rolling, adhesion, and migration as well as vascular permeability were assessed in rat mesenteric venules using intravital microscopy. Expression of adhesion molecules was quantitated using a double radiolabelled monoclonal antibody (mAb) binding technique in vivo (P-selectin, intercellular cell adhesion molecule type 1 (ICAM-1), and vascular cell adhesion molecule 1 (VCAM-1)) or flow cytometry (CD11a, CD11b, and L-selectin). Ex vivo binding of heparin to neutrophils was assessed by flow cytometry. Results—TNF-á induced a significant increase in leucocyte rolling, adhesion, and migration, and vascular permeability, coincident with a significant increase in expression of P-selectin, ICAM-1, and VCAM-1. Ex vivo assessment of blood neutrophils showed significant upregulation of CD11a and CD11b and significant downregulation of L-selectin within five hours of TNF-á administration. Heparin pretreatment significantly attenuated leucocyte rolling, adhesion, and migration but did not aVect expression of cell adhesion molecules or vascular permeability elicited by TNF-á administration. Binding of heparin was significantly increased on blood neutrophils obtained five hours after TNF-á administration. Preincubation with an anti-CD11b mAb but not with an anti-CD11a or anti-L-selectin antibody significantly diminished heparin binding ex vivo. Conclusions—Our results support the concept that the anti-inflammatory effects of heparin involve attenuation of a CD11b dependent adherent mechanism.