Summary
October 2007, Vol. 8, No. 14, Pages 2247-2265 , DOI 10.1517/14656566.8.14.2247

Expert opinion on available options treating pulmonary arterial hypertension

Robert Naeije†,1,2 & Sandrine Huez3 MD
1Professor and Chairman, Erasme University Hospital, Department of Pathophysiology, Erasme Campus, CP 604, 808, Lennik Road, B-1070 Brussels , Belgium +322 5553322; +322 5554124;
2Consultant, Erasme University Hospital, Department of Cardiology
3Assistant, Erasme University Hospital, Department of Cardiology
Author for correspondence



Until in the early nineties, pulmonary arterial hypertension (PAH) was a uniformly fatal disease, with a median life expectancy of 2.5 years. Uncontrolled studies showed that a small proportion of patients responded to high-dose calcium channel blockers, retrospective studies supported the use of anticoagulant therapy and heart–lung or lung transplantation remained the only option. In 1996, a 3-month randomised, placebo-controlled trial showed that chronic intravenous epoprostenol (synthetic prostacyclin) improved functional state, exercise capacity, haemodynamics, and even survival in patients with idiopathic PAH. Similar benefits were subsequently reported and extended to all PAH categories, and confirmed with more stable prostacyclin analogues administered subcutaneously (treprostinil), by inhalation (iloprost), or even orally (beraprost). In the early 2000s, two randomised controlled trials showed efficacy of the oral intake of the dual endothelin A/B receptor antagonist bosentan. Two selective endothelin-A receptor antagonists, sitaxsentan and ambrisentan, are being developed. Finally, a randomised controlled trial has established the therapeutic efficacy of phosphodiesterase-5 inhibition with sildenafil, introducing a third signalling pathway to be targeted by the pharmacological treatment of PAH. Another phosphodiesterase-5 inhibitor, tadalafil, is already being evaluated. While all these treatments have markedly improved the lives of PAH patients, they have not offered yet a cure of the disease. Multi-drug approaches are now under evaluation, with more ambitious therapeutic goals. Alternative approaches with stem cells, RhoA-Rho-kinase inhibitors, platelet derived growth factor inhibitors and vasoactive intestinal peptides are being considered.

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Forward Links to Citing Articles

Michael J Palmer. (2009) Leads for the treatment of pulmonary hypertension. Expert Opinion on Therapeutic Patents 19:5, 575-592
Online publication date: 1-May-2009.
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Bing Cui, Yu-Si Cheng, De-Zai Dai, Na Li, Tian-Tai Zhang, Yin Dai. (2009) CPU0213, A NON-SELECTIVE ET A /ET B RECEPTOR ANTAGONIST, IMPROVES PULMONARY ARTERIOLAR REMODELING OF MONOCROTALINE-INDUCED PULMONARY HYPERTENSION IN RATS. Clinical and Experimental Pharmacology and Physiology 36:2, 169-175
Online publication date: 1-Mar-2009.
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H Kozłowska, M Baranowska, E Schlicker, M Kozłowski, J Laudañski, B Malinowska. (2009) Virodhamine relaxes the human pulmonary artery through the endothelial cannabinoid receptor and indirectly through a COX product. British Journal of Pharmacology 155:7, 1034-1042
Online publication date: 1-Jan-2009.
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Gökhan Tunçbilek, Petek Korkusuz, Figen Özgür. (2008) Effects of Iloprost on Calvarial Sutures. Journal of Craniofacial Surgery 19:6, 1472-1480
Online publication date: 1-Dec-2008.
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O. Kowal-Bielecka, M. Delcroix, A. Vonk-Noordegraaf, M. M. Hoeper, R. Naeije. (2008) Outcome measures in pulmonary arterial hypertension associated with systemic sclerosis. Rheumatology 47:Supplement 5, v39-v41
Online publication date: 1-Nov-2008.
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C. Lafaras, E. Mandala, E. Verrou, D. Platogiannis, N. Barbetakis, T. Bischiniotis, K. Zervas. (2008) Non-thromboembolic pulmonary hypertension in multiple myeloma, after thalidomide treatment: A pilot study. Annals of Oncology 19:10, 1765-1769
Online publication date: 2-Jul-2008.
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Katherine F Croom, Monique P Curran. (2008) Sildenafil. Drugs 68:3, 383-397
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Authors:
Robert Naeije
Sandrine Huez
Keywords:
endothelin receptor antagonist
phosphodiesterase-5 inhibitor
prostacyclin
pulmonary arterial hypertension
septostomy
transplantation