Coronary Artery Disease Clinical Trial
Official title:
Randomized Double-Blind Placebo-Controlled Study of Pyrazinoylguanidine Hydrochloride (Amiloride) in Subjects With Coronary Artery Disease
Treatment of coronary artery disease is a major health care problem across the entire word,
and the United States. Unfortunately, despite a number of medical advances, diagnostic
procedure, or epidemiological studies, the treatment of these patients remain complex, and
and at times frustrating. In fact, the COURAGE trial conducted in 50 centers across United
States and Canada documented that drug treatment, coronary interventions or both were not
effective solution in coronary artery diseases.
A novel approach has recently been developed, based on the critical role of the potassium
(K) content in red-blood-cell in myocardial oxygenation, since oxygen and K binding by
hemoglobin (red-blood-cell) occurs simultaneously in blood passing through the lungs,
whereas in the organs as the heart, the hemoglobin release both Oxygen and K ions.
This apparently simple mechanisms occurs in human blood in all individuals but could be
altered in subjects with acquired or hereditable defect in red-blood-cell K content, as in
hypertensives or CAD patients.
Treatment of Cardiovascular Diseases (CVD) is a major health care problem across the entire
word, and particularly in the United States. In fact, these life-threatening disorders are a
major cause of emergency medical care and hospitalization in the United States, and
according the National Center for Health Statistics (NCHS) there were approximately
1,565,000 hospitalizations for primary or secondary diagnosis of an acute coronary syndrome
(ACS), 669,000 for unstable angina (UA) and 896,000 for myocardial infarction (MI). In the
2003, NCHS reported 4,497,000 visits to emergency departments for primary diagnosis of CVD,
wherein the average age of a person having a first heart attack is calculated at 65.8 years
for men and 70.4 years for women.
Further studies provided by the Heart Disease and Stroke Statistics—2007 Update, of the
American Heart Association, reported an estimated 79 400 000 American adults (1 in 3) have 1
or more types of CVD. Of these, and 37 500 000 are estimated to be age 65 or older. As a
separate diagnosis, high blood pressure or hypertension, accounts for approximately 72 000
000 of patients (defined as systolic pressure 140 mm Hg or greater and/or diastolic pressure
90 mm Hg or greater, taking antihypertensive medication), coronary heart disease (CHD) for
approximately 15 800 000 patients, myocardial infarction for approximately 7 900 000
patients, and angina pectoris (chest pain secondary to ischemic heart disease) for
approximately 8 900 000 patients.
Although the treatment of angina (chest pain secondary to ischemic heart disease and one of
the most common and early symptom of coronary artery disease) can be tracked as far as
1880's, it still represents a medically unresolved problem. Indeed, treatment of angina in
particular, as well as associated condition as ACS, UA, and MI, involves a large number of
life-style change recommendations, dietetic advice, drugs, coronary artery intervention, or
coronary bypass surgery aimed to improve symptoms, quality of life of patients, and even
primary or secondary prevention of the CVD. Unfortunately, despite a century of medical
advances and epidemiological studies, the current approach to CVD, and coronary artery
disease remain complex, and at times frustrating.
Among some of the proposals to combat CVD, have included the single "polypill"(aspirin +
statin + 3 blood pressure lowering agents in half dose, and folic acid) as a strategy to
reduce CVD by more than 80% remains presently unresolved, regression of coronary
atherosclerosis by using Simvastatin and intravascular ultrasound study was determined to be
unpractical. It remains to be determined whether these changes will translate to meaningful
reductions in clinical events, or whether new antithrombotic agents for these CVD patients
can provide an adequate solution. However, the overarching determination in view of the
purported successes to date remains whether these results in highly selected patient
populations can be matched to the real-world treatment of acute coronary syndromes.
In a recent study called the COURAGE Trial (Clinical Outcomes Utilizing Revascularization
and Aggressive Drug Evaluation) conducted in 50 hospital centers across the United States
and Canada showed that optimal drug treatment with percutaneous coronary interventions (PCI)
for stable coronary artery disease, was not more effective than optimal medical therapy
alone for preventing cardiovascular events, hospitalization or death, suggesting that drugs,
surgical procedures or both were not a statistically effective solution for CHD.
For more than a century, hemodynamic mechanisms involving the coupled tissue O2/CO2 gas
exchange and ion H/K transport by Hemoglobin (Hb) in red blood cells (RBC) have been well
known to the scientific community, and has been termed the so-called Bohr/Haldane Effect.
Data to date has been shown that the RBC has a number of critical roles in maintaining
normal vascular function, blood flow, tissue oxygenation and acid-base regulation. These
critical roles, including the nitric oxygen (NO) transport, NO synthetase expression,
platelet aggregation, vascular rheology, and endothelial function, have been the subject of
extensive studies by many investigators. Unfortunately, and despite such multiple integrated
functions to maintain tissue oxygenation in health and diseases states, the role of RBC has
never been of interest in the therapeutic approach of patients with CHD, specially the
ischemic condition of ACS, UA or MI.
In this context, the evidence from our laboratory that erythrocytes have a critical role in
body K homeostasis, along with the finding of a hereditable defect in erythrocyte K uptake
in hypertensives, and 46% of their normotensive (adolescents, young adults) offspring, led
us to assess whether a defective K uptake could impair the regulation of H/K exchange and
oxygen delivery in CAD. Since then, a Patent Application whose filed in the USPTO,and a
simple medical device for intracellular K measurement in red blood cell by miniature K and
Na ion-selective electrode was proposed in conjunction with the University of Michigan.
Although many drugs were tested in order to improve or correct the defective red cell K
transport, the most promising compound was the 3,5-diamino-6-chloro-N-
[diaminomethylene]pyrazinecarboxamide dihydrate derivative, amiloride hydrochloride recently
published as a new drug patent application.
The drug originally tested in hypertensives with low RBC K uptake, independently of cell Na
content, dietary intake or drugs, became an effective and predictable method to improve RBC
K homeostasis that is critically related to other red-cell functions, such as the pH
regulation and oxygen delivery. More important, the observation that reversal of the
abnormal RBC K content was associated with a decline and better control of BP, fasting
plasma glucose, and regression of ST-T alteration related to LVH or CHD, led us to evaluate
the role of RBC in the mechanism of H/K exchange, tissue oxygenation in health and disease
states.
This Clinical Trial will address the effects of Amiloride in RBC K uptake, and consequently
the simultaneous tissue H/K and O2/CO2 exchange, its therapeutic effect on BP control and
possible improvement on Angina, Duke Treadmill Score, and ST-T alteration of LVH or CAD.
METHODS OF TREATMENT
Each patient will be prospectively evaluated in order to assess the effects of Amiloride on
reversion of angina and ECG alterations of ischemia in CAD. After written consent, the
subject will enter the Double-Blind trial of Amiloride Vs Placebo along whit the optimal
treatment for Angina and CHD. Amiloride (5 to 10 mg) will be given daily, before breakfast,
while other medication for angina, and associated diseases as hypertension or diabetes, were
continued. Each patient will be clinically evaluated for angina, dyspnea, or arrhythmias at
1-week, 1, 3, 6 months period. Serial ECG, Ion Transport Studies, BIA, non-invasive
hemodynamic and clinical biochemistry will be obtained at 1, 3, 6 months follow-up period.
Echocardiograms were obtained basal and 6- months period. In this trial, each subject with
plasma ionized calcium (≤1.0 mmol/l) will received 1g of Ca- gluconolactate until the level
was ≥1.0 mmol/l.
Following the first 3-month trial, patients with reversion of angina and improvement of ECG
abnormalities of ischemia will have low doses of amiloride (5 to 7.5 mg), while nitrates,
B-blockers or Calcium Channel Blockers will be progressively discontinued, if no evidence of
angina occurred, and if no new no ECG ST-T alteration of ischemia developed. Therefore,
amiloride with/without aspirin, Statins and medication for hypertension or diabetes, will be
the established treatment until the end of trial.
;
Allocation: Randomized, Endpoint Classification: Safety/Efficacy Study, Intervention Model: Parallel Assignment, Masking: Double Blind (Subject, Investigator), Primary Purpose: Treatment
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