Aortic Stenosis and PhosphodiEsterase Type 5 iNhibition (ASPEN): A Pilot Study



Status:Recruiting
Conditions:Cardiology, Orthopedic
Therapuetic Areas:Cardiology / Vascular Diseases, Orthopedics / Podiatry
Healthy:No
Age Range:18 - Any
Updated:4/21/2016
Start Date:December 2012
End Date:December 2016
Contact:Brian R. Lindman, MD
Email:blindman@dom.wustl.edu
Phone:(314) 747-3617

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Currently, aortic stenosis (AS) is considered a "surgical disease" with no medical therapy
available to improve any clinical outcomes, including symptoms, time to surgery, or
long-term survival. Thus far, randomized studies involving statins have not been promising
with respect to slowing progressive valve stenosis. Beyond the valve, two common
consequences of aortic stenosis are hypertrophic remodeling of the left ventricle (LV) and
pulmonary venous hypertension; each of these has been associated with worse heart failure
symptoms, increased operative mortality, and worse long-term outcomes. Whether altering LV
structural abnormalities, improving LV function, and/or reducing pulmonary artery pressures
with medical therapy would improve clinical outcomes in patients with AS has not been
tested. Animal models of pressure overload have demonstrated that phosphodiesterase type 5
(PDE5) inhibition influences nitric oxide (NO) - cyclic guanosine monophosphate (cGMP)
signaling in the LV and favorably impacts LV structure and function, but this has not been
tested in humans with AS. Studies in humans with left-sided heart failure and pulmonary
venous hypertension have shown that PDE5 inhibition improves functional capacity and quality
of life, but patients with AS were not included in those studies. The investigators
hypothesize that PDE5 inhibition with tadalafil will have a favorable impact on LV structure
and function as well as pulmonary artery pressures. In this pilot study, the investigators
anticipate that short-term administration of tadalafil to patients with AS will be safe and
well-tolerated.

Subjects with moderately severe to severe aortic stenosis (AS), left ventricular hypertrophy
(LVH), diastolic dysfunction, preserved ejection fraction, and no planned aortic valve
replacement over the next 6 months will be eligible for this randomized, double-blind,
placebo-controlled, pilot study. There will be a diabetic cohort (n=32) and non-diabetic
cohort (n=24); each cohort will be randomized 1:1 to tadalafil vs. placebo. During a
baseline study visit, the following will be obtained: clinical data, 6 minute walk, quality
of life questionnaire, blood draw, and an echocardiogram. A 3-day run-in will occur to
initially assess tolerability and compliance. If the drug is tolerated during this run-in
period, participants will be randomized. An MRI will also be performed during this
randomization visit. Follow-up study visits and testing will occur at 6 and 12 weeks and 6
months.

Inclusion Criteria:

- Patients with moderate to severe aortic stenosis (AVA < 1.5 cm2)

- Left ventricular hypertrophy

- Diastolic dysfunction as evidenced by tissue Doppler e' (average of septal and
lateral) ≤ 7 cm/s

- EF ≥ 50%

- None or minimal symptoms related to aortic stenosis (NYHA ≤ 2)

- The subject and treating physician are not planning on a valve replacement procedure
to occur during the next 6 months

- Ambulatory

- Normal sinus rhythm

- 18 years of age and older

- Able and willing to comply with all the requirements for the study

Exclusion Criteria:

- Need for ongoing nitrate medications

- SBP < 110mmHg or MAP < 75mmHg

- Moderately severe or severe mitral regurgitation

- Moderately severe or severe aortic regurgitation

- Contraindication to MRI

- Creatinine clearance < 30 mL/min

- Cirrhosis

- Pulmonary fibrosis

- Increased risk of priapism

- Retinal or optic nerve problems or unexplained visual disturbance

- If a subject requires ongoing use of an alpha antagonist typically used for benign
prostatic hyperplasia (BPH) (prazosin, terazosin, doxazosin, or tamsulosin), SBP <
120 mmHg or MAP < 80 mmHg is excluded

- Need for ongoing use of a potent CYP3A inhibitor or inducer (ritonavir, ketoconazole,
itraconazole, rifampin)

- Current or recent (≤ 30 days) acute coronary syndrome

- O2 sat < 90% on room air

- Females that are pregnant or believe they may be pregnant

- Any condition which the PI determines will place the subject at increased risk or is
likely to yield unreliable data

- Unwilling to provide informed consent
We found this trial at
1
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St. Louis, Missouri 63108
Phone: 314-747-3617
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St. Louis, MO
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