Pulmonary Arterial Hypertension Clinical Trial
Official title:
Effects of Iloprost Treatment in Adult Patients With Pulmonary Arterial Hypertension Related to Congenital Heart Disease (Eisenmenger Physiology): Safety, Tolerability, Clinical, and Hemodynamic Effect.
The prevalence of PAH associated with congenital systemic-to-pulmonary shunts in Western
countries has been estimated to range between 1.6 and 12.5 cases per million adults, with
25-50% of this population affected by Eisenmenger's syndrome. The rarity of this syndrome,
combined with its complex pathophysiology, account for the insufficient understanding of the
principles underlying its proper treatment.Recent decades have seen developments in
pulmonary hypertension pathophysiology which have led to the introduction of new groups of
drugs: prostacycline analogs (Epoprostenol, Treprostinil, Beraprost, Illoprost),
phosphodiesterase inhibitors (Sildenafil, Tadalafil), endothelin receptor antagonists
(Bosentan, Sitaxantan, Ambrisentan) and nitric oxide. These drugs should be administered to
patients in III-IV NYHA class. Despite successful early results, the therapeutic effect on
patients with Eisenmenger syndrome has not been conclusively established The treatment
strategy for patients with PAH associated with congenital systemic-to-pulmonary shunts and,
in particular, those with Eisenmenger's syndrome is based mainly on clinical experience
rather than being evidence based. Although Eisenmenger's syndrome is uncurable disease, the
survival rate is relatively higher than primary PAH, and the patients with Eisenmenger's
syndrome are relatively younger group. So the improvement of exercise tolerance and quality
of life is very important. Several randomized controlled trial reported favourable short-
and long-term outcomes of treatment with the orally active dual endothelin receptor
antagonist bosentan in patients with Eisenmenger's syndrome. However, there was scare data
of outcomes of treatment with the inhaled iloprost in patients with Eisenmenger's syndrome.
In Korea, most of patients with Eisenmenger's syndrome are treated with conservative therapy
instead of administration of PAH-specific drug, because of lack of clinical experience.
Moreover, oral agent such as bosentan, sidenafil is preferred than iloprost becase of more
evidence and convenience. Our therapeutic efforts should be directed mainly towards
preventing complications. As a rule, we should avoid agents with no established therapeutic
efficacy and try to alleviate symptoms without any additional risk, so as not to disrupt the
existing clinical balance.
In this study, we investigate to know the clinical benefit of iloprost on patients with
Eisenmenger's syndrome by the use of functional and hemodynamic parameters, which would add
the evidence of PAH-specific agents on the Eisenmenger's syndrome
A large proportion of patients with congenital heart disease (CHD), in particular those with relevant systemic-to-pulmonary shunts, will develop pulmonary arterial hypertension (PAH) if left untreated. Persistent exposure of the pulmonary vasculature to increased blood flow, as well as increased pressure, may result in pulmonary obstructive arteriopathy, which leads to increased pulmonary vascular resistance that, if it approaches or exceeds systemic resistance, will result in shunt reversal. Eisenmenger's syndrome, the most advanced form of PAH associated with CHD, is defined as CHD with an initial large systemic-to-pulmonary shunt that induces severe pulmonary vascular disease and PAH, with resultant reversal of the shunt and central cyanosis. The histopathological and pathobiological changes seen in patients with PAH associated with congenital systemic-to-pulmonary shunts, such as endothelial dysfunction of the pulmonary vasculature, are considered similar to those observed in idiopathic or other associated forms of PAH. ;
Observational Model: Case-Only, Time Perspective: Prospective
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