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Vol. 303, Issue 2, 741-745, November 2002
Department of Internal Medicine, Justus-Liebig-University, Giessen,
Germany
Iloprost is a potent prostacyclin analog, which has been shown to exert
beneficial effects in several vascular disorders. Inhalation of
aerosolized iloprost was found to cause selective pulmonary
vasodilatation, and this approach is under current investigation for
treatment of chronic pulmonary hypertension. The present study investigated pharmacokinetics and metabolism of aerosolized iloprost in
isolated buffer-perfused rabbit lungs, compared with intravascular administration of the prostanoid. After buffer admixture of iloprost, a
steady decline of perfusate concentrations of the intact prostanoid was
noted (half-life ~3.5 h), mostly attributable to progressive metabolism to dinor- and tetranoriloprost. Inhaled iloprost rapidly entered the intravascular compartment, with peak buffer concentrations being noted after 30 min (bioavailability ~63%). Compared with infused iloprost, significantly more rapid metabolism to dinor- and
tetranoriloprost was noted for iloprost administered via the inhalative
route of application. However, the percentage of the nebulized agent
that enters the intravascular space as intact iloprost displays the
same clearance rate as directly perfusate-admixed prostanoid. We
conclude that a high percentage of inhaled iloprost rapidly enters the
intravascular compartment in intact rabbit lungs. The lung is capable
of metabolizing iloprost via
-oxidation, and more rapid appearance
of dinor- and tetranoriloprost is noted for the inhalative as compared
with the intravascular route of iloprost administration.
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H. Olschewski, B. Rohde, J. Behr, R. Ewert, T. Gessler, H. A. Ghofrani, and T. Schmehl Pharmacodynamics and Pharmacokinetics of Inhaled Iloprost, Aerosolized by Three Different Devices, in Severe Pulmonary Hypertension Chest, October 1, 2003; 124(4): 1294 - 1304. [Abstract] [Full Text] [PDF] |
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