Pulmonary Hypertension Clinical Trial
Official title:
Are Left Ventricular Abnormalities Associated With Pulmonary Hypertension in Sickle Cell Anemia?
This study will explore what may cause people with sickle cell anemia to have heart problems
and an increased risk of sudden death.
People 18 years of age and older with sickle cell anemia may be eligible for this study.
Candidates are screened with a medical history and physical examination, electrocardiogram
(EKG), echocardiogram (heart ultrasound), and blood tests.
Participants undergo the following tests and procedures:
- Holter monitoring: The patient wears a small, battery-operated device to record heart
rate and rhythm over 24 to 48 hours.
- QRST surface mapping: An EKG using 64 electrodes is done at rest and during exercise to
provide a detailed look at the heart and its conduction system.
- Chest x-rays are taken to examine the lungs.
- Bicycle exercise echocardiography test: Blood pressure, pulse, heart rhythm and oxygen
use are monitored while the patient exercises on a stationary bicycle. Ultrasound
pictures are also obtained during the exercise.
- Echocardiogram: A heart ultrasound is done to check how well the heart is pumping blood.
- Pulmonary artery catheterization: A catheter (plastic tube) is inserted into a vein and
advanced to the chambers of the heart, through the heart valve and into the lung artery.
The pressures in the heart and lung blood vessels are measured while the patient is
resting and during exercise, with the bed tilted up and down, and after giving 500 mls
of fluid into a vein.
- Blood tests are done to measure a hormone called brain natriuretic peptide, which can
increase with the development of heart failure, and nitrite, a substance that can affect
blood vessel dilation. Some blood is stored to test for inflammatory markers and for
possible future gene and protein analysis.
- Cardiac magnetic resonance imaging (cMRI): The patient lies in a donut-shaped magnet
while pictures of the heart are obtained using a magnetic field and radio waves.
Earplugs are worn to muffle the loud sounds that occur with electrical switching of the
magnetic fields. A contrast agent called gadolinium may be injected to enhance the
quality of the images.
- Invasive electrocardiographic (reveal) monitoring: This procedure permits study of the
heart rhythms over a long time period. A small device is placed just under the skin on
the left side of the chest. It can be left in for up to 14 months to monitor the
heartbeat continuously during this time.
Sickle cell anemia is an inherited blood disorder primarily affecting groups with origins in
endemic malarial areas, especially those of African descent. SCA results from one of two
single amino-acid substitutions in beta-hemoglobin (Hb-S and Hb-C) that increases the
propensity for hemoglobin to polymerize, thus distorting, sickling and hemolyzing red cells.
Individuals homozygous for Hb-S (or double heterozygote Hb-S and Hb-C) develop sickle cell
anemia (SCA), while heterozygotes have sickle cell trait. SCA is characterized by chronic
anemia and crises of red cell sickling and ischemia that are often painful and affect several
organs and tissue types. SCA confers considerable disability, morbidity and mortality.
Annual mortality from SCA has been estimated at approximately 3%. As a significant number of
these deaths are sudden, a cardiac cause has been suspected. However, no cardiac mechanism of
sudden death (SD) has been clearly identified. Recently, it has been demonstrated that SCA
patients with pulmonary hypertension (PAH) have a higher incidence of SD than those with
normal pulmonary pressures. In many patients, PAH occurs in association with elevated
pulmonary arterial wedge pressures and normal pulmonary arterial resistance, suggesting that
the PAH develops as the result of left ventricular (LV) abnormalities. Furthermore, in other
conditions in which PAH develops, SD occurs only at pressures considerably higher than those
observed in SCA. These factors suggest that PAH in SCA is a surrogate marker for, rather than
the cause of SD. Rather, an SCA cardiomyopathic process may provide a unifying mechanism that
associates moderate degrees of PAH and high risk of SD from cardiac causes.
We propose to describe the extent of cardiac involvement in SCA. Specifically, we will (1)
describe the LV volume-pressure relations in SCA patients with and without pulmonary
hypertension in order to determine how elevated pulmonary pressures are related to dynamic
filling properties of the LV; and (2) determine whether cardiac arrhythmias are common in SCA
patients with PAH and if they contribute to SD.
Improved understanding of the etiology and mechanisms of SD in SCA may allow the development
and testing of therapies for the primary prevention of SD.
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