APA
Murciano, Juan Carlos & Muro, Silvia & Koniaris, Lauren & Christofidou-Solomidou, Melpo & Harshaw, David W. & Albelda, Steven M. & Granger, D. Neil & Cines, Douglas B. & Muzykantov, Vladimir R. (2003 ) .ICAM-directed vascular immunotargeting of antithrombotic agents to the endothelial luminal surface.
ISO 690
Murciano, Juan Carlos & Muro, Silvia & Koniaris, Lauren & Christofidou-Solomidou, Melpo & Harshaw, David W. & Albelda, Steven M. & Granger, D. Neil & Cines, Douglas B. & Muzykantov, Vladimir R.. 2003 .ICAM-directed vascular immunotargeting of antithrombotic agents to the endothelial luminal surface.
https://hdl.handle.net/20.500.12080/39704
Abstract:
Drug targeting to a highly expressed,
noninternalizable determinant up-regulated
on the perturbed endothelium may help to
manage inflammation and thrombosis. We
tested whether inter-cellular adhesion mole cule-1 (ICAM-1) targeting is suitable to de liver antithrombotic drugs to the pulmonary
vascular lumen. ICAM-1 antibodies bind to
the surface of endothelial cells in culture, in
perfused lungs, and in vivo. Proinflamma tory cytokines enhance anti-ICAM binding
totheendotheliumwithoutinducinginternal ization. 125I-labeled anti-ICAM and a reporter
enzyme( -Gal)conjugatedtoanti-ICAMbind
to endothelium and accumulate in the lungs
after intravenous administration in rats and
mice. Anti-ICAM is seen to localize predomi nantly on the luminal surface of the pulmo nary endothelium by electron microscopy.
We studied the pharmacological effect of
ICAM-directed targeting of tissue-type plas minogen activator (tPA). Anti-ICAM/tPA, but
not control IgG/tPA, conjugate accumulates
in the rat lungs, where it exerts plasminogen
activator activity and dissolves fibrin micro emboli. Therefore, ICAM may serve as a
target for drug delivery to endothelium, for
example, for pulmonary thromboprophy laxis. Enhanced drug delivery to sites of
inflammation and the potential anti-inflam matory effect of blocking ICAM-1 may en hance the benefit of this targeting strategy