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Arteriosclerosis, Thrombosis, and Vascular Biology. 2005;25:723-728
Published online before print January 27, 2005, doi: 10.1161/01.ATV.0000157578.51417.6f
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(Arteriosclerosis, Thrombosis, and Vascular Biology. 2005;25:723.)
© 2005 American Heart Association, Inc.


Vascular Biology

Powerful Inflammatory Properties of Large Vein Endothelium In Vivo

Einar E. Eriksson; Eva Karlof; Karin Lundmark; Pierre Rotzius; Ulf Hedin; Xun Xie

From the Department of Physiology and Pharmacology (E.E.E., E.K., P.R., X.X.), Karolinska Institutet, and the Department of Surgical Sciences (K.L., U.H.), Division of Vascular Surgery, Karolinska Hospital, Stockholm, Sweden.

Correspondence to Einar Eriksson, Department of Physiology and Pharmacology, Karolinska Institutet S-171 77 Stockholm, Sweden. E-mail einar.eriksson{at}fyfa.ki.se

Objective— Inflammatory responses of large vein endothelium are of importance in pathological processes such as venous thrombosis, chronic venous congestion, and vein graft atherosclerosis. However, the inflammatory properties of large vein endothelium are unclear.

Methods and Results— In this study, we used several microscopy techniques to investigate the inflammatory properties of large vein endothelium in vivo. We show that the endothelium in the mouse inferior vena cava (IVC) possesses powerful inflammatory properties that are distinct from the less inflammatory reactive aortic endothelium and virtually identical to endothelial responses in postcapillary venules. Inflammatory stimulation with tumor necrosis factor-{alpha} induced strong expression of cell adhesion molecules (CAMs) in the IVC. These CAMs promoted recruitment of leukocytes, platelets, and erythrocytes to the vein wall. The inflammatory responses altered endothelial structure and increased endothelial permeability in the IVC. Accumulation of blood cells and endothelial damage were markedly reduced in mice deficient in the endothelial leukocyte recruitment molecules E-selectin and P-selectin, indicating a central role for these molecules in driving structural and functional changes of IVC endothelium.

Conclusions— These findings provide the first comprehensive demonstration of the inflammatory capacity of large vein endothelium and emphasize the actions of endothelial cells as targets in large vein disease.

The inflammatory capacity of large vein endothelium is unclear. Here, we show that endothelium in the mouse IVC holds powerful inflammatory properties that are equally potent as that in postcapillary venules and distinct from that in arteries. The data emphasize the endothelium as target for treatment of vein disease.


Key Words: endothelium • leukocyte • rolling • adhesion • vein • inflammation




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