Imatinib and Carvedilol for High Blood Pressure in the Lungs in Adults With Sickle Cell Disease
Status: | Completed |
---|---|
Conditions: | High Blood Pressure (Hypertension), Anemia |
Therapuetic Areas: | Cardiology / Vascular Diseases, Hematology |
Healthy: | No |
Age Range: | Any |
Updated: | 11/18/2012 |
Start Date: | March 2012 |
End Date: | February 2014 |
Contact: | Catherine A Seamon, R.N. |
Email: | cseamon@cc.nih.gov |
Phone: | (301) 451-6313 |
A Pilot Study of Treatment of Adults With Sickle Cell Disease Associated Pulmonary Hypertension Based on Hemodynamic Stratification: Safety and Tolerability Study of Imatinib and Carvedilol
Background:
- About one-tenth of adults with sickle cell disease have pulmonary hypertension (high blood
pressure in the lungs). This condition can cause shortness of breath, pain crisis, and
congestive heart failure. It may even lead to death. Researchers want to test the drugs
imatinib and carvedilol to see if they can treat high blood pressure in the lungs. Both
drugs have been used to treat other types of heart problems, but they have not been tested
as a treatment for high blood pressure related to sickle cell disease.
Objectives:
- To see if imatinib and carvedilol are safe and effective treatments for high blood
pressure in the lungs in adults with sickle cell disease.
Eligibility:
- Adults at least 18 years of age who have sickle cell disease and have or may have high
blood pressure in the lungs.
Design:
- Participants will be screened with a physical exam and medical history. They will also
have different tests of heart and lung function, including a walking test and imaging
studies. Blood and urine samples will also be collected.
- Participants who meet specific criteria will take one of two possible study drugs.
Those who receive imatinib will take it daily. Those who receive carvedilol will take
it twice a day.
- Participants will have weekly study visits for blood tests and other exams. The study
drug dose will be adjusted at each weekly visit. It will be increased slowly to reach a
target dose(based on the participant's weight) or to find a stable effective dose.
- Participants may continue to take their study drug for up to 24 weeks, with weekly
study visits. Regular blood samples and heart and lung function tests will be
performed.
- After 24 weeks, qualified participants may continue to take their study drug for up to
6 more months. They will have regular study visits to monitor the treatment.
Sickle Cell Disease related pulmonary hypertension is a heterogeneous condition that results
in a high mortality and for which no therapy has been documented to be beneficial. We
propose to perform a safety and tolerability study of treatments based on right heart
catheterization derived hemodynamic profiles associated with higher mortality in our cohort.
These same hemodynamic profiles have previously been described and confirmed in other large
cohorts as well. We propose treatment of sickle cell subjects with pulmonary arterial
hypertension (PAH), defined hemodynamically by pulmonary arterial mean pressures (mPAP) of
25 mmHg or greater, with low estimated left ventricular filling pressures (low pulmonary
capillary wedge pressures, or PCWP), and high pulmonary vascular resistance (PVR), with
imatinib, a tyrosine kinase inhibitor that modifies the Platelet Derived Growth Factor
(PDGF) pathway. PDGF is involved in Sickle Cell related PAH and there is now evidence that
imatinib is effective in the treatment of idiopathic PAH. The hemodynamic profile of
elevated mPAP with elevated left ventricular filling pressures is also associated with
higher mortality rates, and we propose to treat this subgroup with carvedilol, a unique
beta-adrenergic receptor antagonist that has been demonstrated to attenuate the adrenergic
response and improve right and left heart function. The third subgroup with elevated mPAP
is the hyperdynamic group, which by definition has low PVR and the absence of elevated left
ventricular filling pressures. This group is also at higher risk but over a longer period
of time and for less evident reasons. We will continue with aggressive sickle cell
management in the hyperdynamic group according to the expertise offered by the Sickle Cell
Group at the Clinical Center while systematically following them and intervening with
optimal care. Those who do not quality for any of the three subgroups described above will
go into a fourth subgroup and be followed for mortality and data sharing. Our primary
endpoint is the safety and tolerability of these interventions and our secondary endpoints
will be the clinical efficacy of these treatments.
- Eligibility Criteria
- Subjects 18 years of age or older
- Must be able to provide written informed consent
- Subjects with SCD and prior RHC documenting mPAP greater than or equal to 25 mmHg
- Suspicion of Pulmonary Hypertension based on any of the below criterion:
- exertional breathlessness
- echocardiographic evidence of tricuspid insufficiency (TRVgreater than or equal to
2.7 m/s)
- oxy-hemoglobin desaturation during six minute walking test
- hypoxia requiring supplemental oxygen
- pedal edema
- ascites
- elevated BNP
- or history of acute chest syndrome, stroke, or other serious complication of
vaso-occlusive disease
- history of chest pain, syncopal events or thromboembolic events
- The referring physician may refer the subject for other suspicious symptoms or
findings of SCD-PH
INCLUSION CRITERIA:
Arm A (Imatinib)
1. Satisfaction of screening criteria
2. Subjects 18 years of age or older
3. Women of childbearing potential and male subjects must agree to use reliable methods
of birth control (oral contraceptives, other hormonal contraceptives including
vaginal contraceptive rings and contraceptive patches, barrier contraceptives such as
condoms, an intra uterine device (IUD) or abstinence). This is because the effects
of imatinib mesylate on the developing human fetus are not fully known.
4. Diagnosis of sickle cell disease (electrophoresis or HPLC)
5. Documentation of SS, SC, S-Beta thalassemia or other major sickling phenotypes)
6. Diagnosis of sickle cell disease associated pulmonary hypertension by right heart
catheterization (mean PAP greater than or equal to 25 mmHg AND PCWP less than or
equal to 15 mmHg with PVR greater than or equal to 3.0 Wood's Units)
7. WHO functional class II or III symptoms
Arm B (Carvedilol)
1. Satisfaction of screening criteria
2. Right heart catheterization (mean PAP greater than or equal to 25 mmHg AND PCWP > 15
mmHg
3. Clinically stable for at least 6 weeks prior to enrollment. PAH treatments must be
stable for three months prior to study drug initiation. Prostacyclin analogs, type 5
phosphodiesterase inhibitors and endothelin-1 receptor antagonists are all allowed,
alone or in combinations
4. Diagnosis of sickle cell disease (electrophoresis or HPLC documentation of SS, SC,
S-Beta thalassemia or other major sickling phenotypes)
5. Women of childbearing potential and male subjects must agree to use reliable methods
of birth control (oral contraceptives, other hormonal contraceptives including
vaginal contraceptive rings and contraceptive patches, barrier contraceptives such as
condoms, an intra uterine device (IUD) or abstinence). This is because the effects
of Carvedilol in pregnancy is unknown (pregnancy risk factor C).
6. Subjects 18 years of age or older
7. WHO functional class II or III symptoms
Arm C (Hyperdynamic)
1. Sickle cell disease
2. Diagnosis of sickle cell disease associated pulmonary hypertension by right heart
catheterization (mean PAP greater than or equal to 25 mmHg AND PCWP less than or
equal to 15 mmHg with PVR < 3.0 Wood's Units)
3. Subjects 18 years of age or older
Arm D
1) Don't qualify for Arm A, B, or C after completing the baseline assessments.
EXCLUSION CRITERIA
Arm A (Imatinib):
1. Current pregnancy and lactation.
2. Life expectancy less than 6 months.
3. WHO functional class IV symptoms or NYHA-IV dyspnea.
4. Presence of any of the medical conditions that are considered to be the cause of
subject's pulmonary hypertension by subject's physician, including but not limited
to:
- Scleroderma.
- Known significant obstructive or restrictive respiratory disease with FEV1, FVC
or TLC below 60 percent of predicted normal.
- Known diagnosis of Obesity-Hypoventilation Syndrome.
- Portal hypertension or Child Class B or C cirrhosis.
- Significant left ventricular dysfunction (LVEF below 50 percent), significant
ischemic, valvular, constrictive or restrictive heart disease.
5. Persistently uncontrolled severe systemic hypertension (SBP above 160 mmHg or DBP
above 100 mmHg)
6. Clinical diagnosis of decompensated congestive heart failure
7. Any initiation of new therapeutic intervention within the last 90 days or a dose
change within 30 days, that is expected to have an impact on pulmonary hypertension,
including but not limited to:
1. Specific pulmonary hypertension medication (e.g. prostacyclin analogues,
endothelin receptor antagonists or phosphodiestrase-5 inhibitors)
2. Hydroxyurea
3. Scheduled blood transfusions or exchange transfusions
8. Any acute or chronic, physical or psychiatric impairment, likely to limit subject's
ability to comply with study requirements as determined by investigators.
9. Subjects having inadequate organ function or hematopoeisis as defined below:
1. Absolute Neutrophil Count (ANC) < 1200/mcL
2. Platelets Count < 50, 000 / mcL
3. ALT (SGPT) > 3 times upper limit of normal
4. Creatinine greater than or equal to 2.0 mg/dl
5. Creatinine Clearance < 60 mL/min/1.73 m sq
10. Subjects enrolled in any other interventional drug trial.
11. History of allergic reaction to compounds with similar chemical or biologic
composition to imatinib.
12. Any know concurrent condition that is likely to confound investigators' ability to
monitor drug related adverse events.
13. Any previous treatment with any Tyrosine Kinase Inhibitor within last 90 days.
14. Any SCD related acute illness requiring hospitalization within two weeks. This will
include but is not limited to:
1. Acute vaso-occlusive pain crisis.
2. Acute chest syndrome
3. Significant upper or lower respiratory tract infection
15. Significant upper or lower respiratory tract infection requiring hospitalization or
emergency department visit within 2 weeks.
16. HIV positive subjects on Highly Active Anti-retroviral therapy (due to potential for
drug interaction as well as severe immunosuppression).
17. Acute pulmonary embolism within the previous 90 days.
Subjects enrolled on this protocol who are excluded due to above criteria may proceed when
their circumstances change to satisfy the exclusion criteria requirements.
Arm B (Carvedilol)
1. Current pregnancy and lactation
2. Life expectancy less than 6 months.
3. WHO functional class IV symptoms or NYHA-IV dyspnea.
4. Presence of the following medical conditions that are considered to be the cause of
subject's pulmonary hypertension:
1. Scleroderma
2. Known significant obstructive or restrictive respiratory disease with FEV1, FVC
or TLC below 60 percent of predicted normal.
3. Known diagnosis of Obesity-Hypoventilation Syndrome.
4. Portal hypertension or any form of severe liver dysfunction.
5. Structural or congenital heart disease felt to be causing the pulmonary
hypertension
5. Decompensated left ventricular failure requiring intravenous inotropic therapy
6. Persistent hypotension (SBP below 90 mmHg or DBP below 50 mmHg).
7. Any subject with baseline heart rate less than or equal to 60 bpm, sick sinus
syndrome, or second or third degree AV block.
8. Any initiation of new therapeutic intervention within the last 90 days or a dose
change within 30 days, that is expected to have an impact on pulmonary hypertension,
including but not limited to:
1. Specific pulmonary hypertension medication (e.g. prostacyclin analogues,
endothelin receptor antagonists or phosphodiestrase-5 inhibitors)
2. Hydroxyurea
3. Scheduled blood transfusions or exchange transfusions
9. Any acute or chronic, physical or psychiatric impairment, likely to limit subject's
ability to comply with study requirements as determined by investigators.
10. Subjects enrolled in any other interventional trial.
11. History of allergic reaction to compounds with similar chemical or biologic
composition to carvedilol
12. Any know concurrent condition that is likely to confound investigators' ability to
monitor drug related adverse events
13. Use of beta-blockers within previous 90 days.
14. Cardiac index < 1.8 l/ min (2)
15. Severe renal insufficiency (creatinine clearance < 30 ml/min/m(2))
16. Any SCD related acute illness requiring hospitalization within two weeks. This will
include but is not limited to:
1. Acute vaso-occlusive pain crisis.
2. Acute chest syndrome
3. Significant upper or lower respiratory tract infection requiring hospitalization
or emergency department visit
17. Significant upper or lower respiratory tract infection requiring hospitalization or
emergency department visit within 2 weeks.
18. HIV positive subjects on Highly Active Anti-retroviral therapy due to potential for
drug interaction.
19. Subjects with active hepatitis infection as the monitoring of drug related liver
toxicity will be confounded.
20. Acute pulmonary embolism within the previous 90 days.
21. Liver function abnormalities (screening serum ALT> 5 times upper limit)
22. Subjects with severe asthma as defined by presence of one or more of the following:
- Presence of asthma symptoms throughout the day
- Nocturnal symptoms every night
- Need for rescue medications several times per day
- Two or more acute exacerbations of asthma requiring systemic steroids therapy
within the preceding year
- A reduced FEV1/FVC ratio or FEV1 below 60 percent of predicted normal.
Subjects enrolled on this protocol that are excluded due to above criteria may proceed
when their circumstances change to satisfy the exclusion criteria requirements.
Arm C (Hyperdynamic)
1) There are no exclusion criteria.
Arm D
1) There are no exclusion criteria.
We found this trial at
1
site
9000 Rockville Pike
Bethesda, Maryland 20892
Bethesda, Maryland 20892
301-496-4000
National Institutes of Health Clinical Center The National Institutes of Health (NIH) Clinical Center in...
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