Pulmonary Hypertension Clinical Trial
Official title:
A Clinical Trial of Ambrisentan and Tadalafil in Pulmonary Arterial Hypertension Associated With Systemic Sclerosis
This will be a 36-week, randomized, double-blind, parallel group study comparing the effects of tadalafil monotherapy, ambrisentan monotherapy and combination therapy with tadalafil and ambrisentan in patients with PAH-SSc. Standard outcome measures such as six-minute walk distance (6MWD), NYHA classification, and hemodynamic measurements will be assessed, as well as novel functional measures of RV-PV function including the transthoracic echocardiogram parameter tricuspid annular plane systolic ejection (TAPSE), contrast-enhanced cardiac MRI and heart rate variability assessed by Holter monitoring. This design (excluding a placebo-placebo arm) was selected for ethical concerns and to provide optimal efficiency and active therapy to all study subjects. It also allows for comparisons between the two monotherapies and with combination therapy.
Pulmonary Arterial Hypertension (PAH) includes a heterogeneous group of clinical entities
sharing similar clinical and pathological features that have been subcategorized as
idiopathic PAH (IPAH, formerly known as "primary pulmonary hypertension" or PPH), familial
PAH, pulmonary hypertension related to connective tissue diseases (such as systemic
sclerosis), portopulmonary hypertension and pulmonary hypertension related to HIV infection,
drugs and toxins (10). PAH is clinically defined by a resting mean pulmonary artery pressure
≥ 25 mmHg and pulmonary artery wedge pressure ≤ 15 mmHg in the absence of left heart
disease, underlying parenchymal lung disease, thromboembolic disease or other causes of
pulmonary hypertension.
PAH is characterized by increased pulmonary vascular resistance due to remodeling and
occlusion of the pulmonary arterioles. Left untreated, PAH leads irremediably to right
ventricular (RV) hypertrophy, pressure overload and dilation resulting in death within 2-3
years (11). For the past two decades, it has been appreciated that the integrity of the RV
function, rather than the degree of pulmonary vascular injury, is the major determinant of
symptoms and mortality in patients with PAH. RV dysfunction at time of presentation, as
reflected by an elevation in right atrial pressure (RAP), the presence of pericardial
effusion or depressed cardiac output (CO), is a powerful prognosticator of death (12).
Current PAH therapies consist of prostacyclin analogues, endothelin receptor antagonists
(ETRA) and phosphodiesterase type V (PDE V) inhibitors (13). All have been shown to be
effective in improving exercise capacity as measured by the 6 MWD in short term (12 - 16
week) randomized, placebo-controlled clinical trials. However, the clinical response is
highly variable and mortality remains high (14). Moreover, the majority of subjects enrolled
in these trials have had IPAH. Over the past 10 years, the Johns Hopkins Pulmonary
Hypertension Program and Scleroderma Center have worked closely to address the daunting
clinical challenge of PAH associated with scleroderma or systemic sclerosis (PAH-SSc).
Previous work from our group (15;16) and others (17-19) has clearly demonstrated a markedly
worse prognosis in PAH-SSc compared with IPAH despite similar treatments. An intriguing and
consistent finding when comparing these two groups is that whereas mPAP is, on average,
lower in PAH-SSc, markers of RV dysfunction (e.g. CO and RAP) are similar, raising the
possibility of maladaptive RV response to pressure overload and/or intrinsic myocardial
disease. Current PAH therapies target pathways that have been implicated in the remodeling
of the pulmonary vasculature (PV). However, there is no clear evidence that these therapies
have altered PV and/or RV remodeling or offered significant beneficial effects in patients
with PAH-SSc in whom mortality remains exceedingly high. In addition, their effects on RV
dysfunction and RV-PV interaction remain poorly characterized.
We hypothesize that improvement in PAH-SSc will only be achieved with therapy directly
targeted at RV-PV dysfunction. Sildenafil and tadalafil inhibit phosphodiesterase type 5
(PDE5) which is abundant in the lung and is the main enzyme responsible for cGMP hydrolysis.
The resulting increase in cGMP probably mediates the relaxant and anti-hypertrophic actions
of nitric oxide and natriuretic peptides in vascular tissues, and exerts a direct
anti-hypertrophic action on cardiac muscle as demonstrated in compelling preliminary
experiments by investigators of the NHLBI-funded Hopkins Scientific Center of Clinically
Oriented Research (SCCOR) in Pulmonary Vascular Disease. In these experiments, sildenafil
was capable of preventing and reversing RV hypertrophy and dysfunction in a model of
pulmonary artery banding, similar to its effects on the left ventricle with aortic banding
(20), indicating a direct beneficial action on RV remodeling.
Both sildenafil (21) and tadalafil (22) have been demonstrated to be effective in PAH and
are FDA approved for this indication. The endothelin-receptor antagonists, bosentan (23) and
ambrisentan (24), are also FDA-labeled for this indication and represent alternative options
for oral therapy of PAH (25). A small randomized study comparing sildenafil with bosentan
suggested that sildenafil was superior in reducing RV mass and improving exercise capacity
in patients with PAH (26). Recently, the results of a large multi-center randomized,
controlled trial of tadalafil therapy for PAH have been presented. The data indicate, that
similar to sildenafil, tadalafil at doses of 20 and 40 mg per day, improved exercise
capacity. In addition, tadalafil 40 mg per day improved pulmonary hemodynamics, quality of
life and reduced the incidence of clinical worsening.
This study aims to compare the effects of tadalafil therapy, ambrisentan therapy and the
combination of both agents in PAH-SSc on PVR and RV mass. It will also assess novel markers
of RV function by cardiac MRI and echocardiography, as well as the conventional endpoints,
including 6 MWD and functional class. The trial is unique in that it will enroll only
PAH-SSc patients, the PAH subgroup with the poorest outcomes and will be considerably longer
in duration (36 weeks) than previous studies. In addition, the effects of first line
combination therapy with an ETRA/PDE V inhibitor will be compared with single agent
regimens.
;
Allocation: Randomized, Endpoint Classification: Safety/Efficacy Study, Intervention Model: Parallel Assignment, Masking: Double Blind (Subject, Caregiver, Investigator, Outcomes Assessor), Primary Purpose: Treatment
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