Pharmacokinetics and Metabolism of Infused versus Inhaled Iloprost in Isolated Rabbit Lungs

Schermuly, Ralph Theo; Schulz, Andreas; Ghofrani, Hossein Ardeschir; Meidow, Arne; Rose, Frank; Roehl, Axel; Weißmann, Norbert; Hildebrand, Michael S.; Kurz, Julia; Grimminger, Friedrich; Walmrath, D.; Seeger, Werner

doi:10.1124/jpet.303.2.741

Cited by 22 publications

(8 citation statements)

References 22 publications

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“…This can be detected by a fall in the PVR/SVR ratio from an initial 0.22 to 0.14 and by the nonlife-threatening but nevertheless significant fall in the mean arterial pressure from 85 mm Hg to 77 mm Hg and a tendential fall in systemic resistance from 1660 to 1390 dyn·s·cm − 5 . The systemic effect is attributable to a spilling over of the substance into the systemic circulation, which would also tally with the results of a lung perfusion study in the isolated rabbit lung [30], using inhaled iloprost, and a comparative study of various nebulizer systems by Olschewski et al [29]. In our study cohort, a marked fall in pulmonary capillary wedge pressure was recorded in some cases on inhaled iloprost as a result of the fall in systemic afterload.…”

Section: Discussionsupporting

confidence: 50%

Evaluation of pulmonary vascular response to inhaled iloprost in heart transplant candidates with pulmonary venous hypertension

Braun

Schrötter

Schmeißer

et al. 2007

International Journal of Cardiology

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Section: Discussionsupporting

confidence: 50%

Evaluation of pulmonary vascular response to inhaled iloprost in heart transplant candidates with pulmonary venous hypertension

Braun

Schrötter

Schmeißer

et al. 2007

International Journal of Cardiology

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“…This difference is most likely due to some species variance in the kinetics of the iloprost catabolic pathway: being chemically stable – in contrast to prostacyclin – iloprost is converted to dinor-and tetranor-iloprost metabolites via beta-oxidation [25]. The liver is known to be a major site of this catabolic pathway, however, recent studies in isolated perfused rabbit lungs demonstrated that the conversion of iloprost to these beta-oxidation products also takes place in the lung tissue itself [26]. …”

Section: Discussionmentioning

confidence: 99%

Lung vasodilatory response to inhaled iloprost in experimental pulmonary hypertension: amplification by different type phosphodiesterase inhibitors

et al. 2005

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Inhaled prostanoids and phosphodiesterase (PDE) inhibitors have been suggested for treatment of severe pulmonary hypertension. In catheterized rabbits with acute pulmonary hypertension induced by continuous infusion of the stable thromboxane analogue U46619, we asked whether sildenafil (PDE1/5/6 inhibitor), motapizone (PDE3 inhibitor) or 8-Methoxymethyl-IBMX (PDE1 inhibitor) synergize with inhaled iloprost. Inhalation of iloprost caused a transient pulmonary artery pressure decline, levelling off within <20 min, without significant changes in blood gases or systemic hemodynamics. Infusion of 8-Methoxymethyl-IBMX, motapizone and sildenafil caused each a dosedependent decrease in pulmonary artery pressure, with sildenafil possessing the highest efficacy and at the same time selectivity for the pulmonary circulation. When combining a per se ineffective dose of each PDE inhibitor (200 µg/kg × min 8-Methoxymethyl-IBMX, 1 µg/kg × min sildenafil, 5 µg/kg × min motapizone) with subsequent iloprost nebulization, marked amplification of the prostanoid induced pulmonary vasodilatory response was noted and the area under the curve of P PA reduction was nearly threefold increased with all approaches, as compared to sole iloprost administration. Further amplification was achieved with the combination of inhaled iloprost with sildenafil plus motapizone, but not with sildenafil plus 8MM-IBMX. Systemic hemodynamics and gas exchange were not altered for all combinations. We conclude that co-administration of minute systemic doses of selective PDE inhibitors with inhaled iloprost markedly enhances and prolongs the pulmonary vasodilatory response to inhaled iloprost, with maintenance of pulmonary selectivity and ventilation perfusion matching. The prominent effect of sildenafil may be operative via both PDE1 and PDE5, and is further enhanced by co-application of a PDE3 inhibitor.

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“…Moreover, SCHERMULY et al [30] showed that inhaled iloprost rapidly enters the intravascular compartment in healthy isolated rabbit lungs. Therefore, a retarded release of iloprost from out of the alveolar space, which might have contributed to a delayed selective vasodilation in the present study, seems to be improbable.…”

Section: ¡158 630¡171mentioning

confidence: 99%

Cardiopulmonary effects of iloprost in experimental acute lung injury

Dembinski

Brackhahn²,

Henzler³

et al. 2005

European Respiratory Journal

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Iloprost, a prostacyclin analogue with a prolonged plasma half-life has beneficial effects in chronic pulmonary hypertension, whereas the effects in acute lung injury (ALI) are unknown. The present study was performed to evaluate the cardiopulmonary effects of iloprost in experimental ALI.ALI was induced in 18 pigs by repeated lung lavage. Animals were randomised to controls, i.v. or inhaled iloprost for 15 min. Haemodynamics, gas exchange and ventilation-perfusion distribution were measured at the end of iloprost application and after 1 and 2 h.As a short-term effect, both i.v. and inhaled iloprost significantly decreased pulmonary artery pressure without major effects on gas exchange or systemic haemodynamics. After 1 and 2 h, a reduction of pulmonary hypertension was no longer present. As a long-term effect, inhaled, but not i.v., iloprost decreased pulmonary shunt and significantly improved gas exchange after 1 and 2 h.In conclusion, the single application of iloprost revealed short-term pulmonary vasodilation without other major cardiopulmonary effects. However, inhaled iloprost improved gas exchange due to a decrease of pulmonary shunt as a long-term effect, possibly as a result of a reduction of lung oedema formation.

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Pharmacokinetics and Metabolism of Infused versus Inhaled Iloprost in Isolated Rabbit Lungs

Cited by 22 publications

References 22 publications

Evaluation of pulmonary vascular response to inhaled iloprost in heart transplant candidates with pulmonary venous hypertension

Evaluation of pulmonary vascular response to inhaled iloprost in heart transplant candidates with pulmonary venous hypertension

Lung vasodilatory response to inhaled iloprost in experimental pulmonary hypertension: amplification by different type phosphodiesterase inhibitors

Cardiopulmonary effects of iloprost in experimental acute lung injury

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