Essential Hypertension Clinical Trial
Official title:
Antihypertensive Effect of Different Doses of Rostafuroxin in Comparison With Losartan, Assessed by Office and Ambulatory Blood Pressure Monitoring in a Hypertensive Population Selected According to a Specific Genetic Profile
The principal aim of the study is to demonstrate that Rostafuroxin is able to induce a more pronounced reduction of arterial blood pressure respect to Losartan, in hypertensive patients carrying at least one of the pre-specified gene mutations. In previous studies has been demonstrated that these mutations are able to induce specific alterations inducing an increase of sodium (Na) reabsorption at renal tubular level and an increase of arterial blood pressure. Pilot studies have demonstrated that Rostafuroxin is able to reduce the impact of these alterations, and so directly reverse the increase in blood pressure.
About 30% of the world adult population is affected by hypertension in industrialised
countries. Elevated arterial pressure is the major cause of cardiovascular mortality and
international guidelines emphasise the benefits of reducing blood pressure. The current
antihypertensive strategies may reduce by 20-30% the cardiovascular risk of hypertensive
patients when this efficacy is measured in clinical trials in comparison with placebo. A
precise world-wide estimation of this efficacy both in term of patient burden and healthcare
costs is not available; however, a recent analysis suggests that the world-wide cost of
hypertension associated cardiovascular complications is around 1,000 billions dollars.
Therefore, effective improvement in the diagnosis and treatment of hypertension can provide
the most significant contribution to the decrease of cardiovascular mortality and reduction
of the world-wide costs associated to treatment of hypertension complications.
Most of clinical trials, performed with the aim to show a reduction of the systolic blood
pressure in hypertensive patients, show that reduction of systolic blood pressure is
independent from the class of tested drugs as diuretics, β blockers, Ca channel blockers or
inhibitors of RAS seem to have roughly the same efficacy. These findings have been used as
an argument to support the notion that the antihypertensive therapy efficacy in reducing
cardiovascular risk depends on the magnitude of the blood pressure fall rather than on the
mechanism of action of the drug. This view contrasts with the well established notion that
the secondary prevention capacity in other cardiovascular diseases differs among these
classes of drugs with minor difference on the prevention of heart failure or stroke between
the Ca antagonist and the other classes of drugs.
Furthermore, the recent findings on genetic of hypertension taken together with the previous
data on pathophysiology of hypertension and its cardiovascular complications are consistent
with the notion that a variety of heterogeneous genetic-molecular mechanisms concur to
develop the rather uniform clinical picture of primary hypertension. Drugs are small
molecules that produce their effects by interacting with larger molecules (proteins) whose
function or reactivity may vary from one patient to another because the variations within
the gene encoding them. Therefore, it is logical to postulate that the consequence of this
different interaction either in term of blood pressure reduction or cardiovascular risk
prevention may vary from a patient to another according to the peculiar function of the
proteins involved in a given patient.
Rostafuroxin was selected during a research program aimed to synthesizing and selecting new
antihypertensive compounds able to interfere with abnormalities in Na tubular reabsorption
due to humoral and/or genetic mechanisms leading to essential (or genetic) hypertension.
Many studies performed on the Milan hypertensive strain of rats (MHS), bearing a primary
renal alteration in the ability to excrete sodium and increased blood pressure levels,
showed a clear capacity of Rostafuroxin to revert these alteration, reducing systemic blood
pressure.
Rostafuroxin selectively interferes with the Na-K pump correcting its functional
abnormalities without interfering with other receptors involved in blood pressure regulation
or hormonal homeostasis. At nanomolar concentration, rostafuroxin reduces the Na-K pump
hyperactivation induced in renal cell cultures by either incubation with nanomolar ouabain
concentrations or cell transfection with the 'hypertensive' variant of adducin.
Similarly, less than 1 μg/kg os of rostafuroxin is able to completely normalize both blood
pressure and the increased renal Na-K pump activity in rats made hypertensive by a chronic
infusion of low-dose ouabain. The antihypertensive effect of rostafuroxin is long-lasting
since it is still present 24 hours after oral administration. It is not associated with
changes in heart rate. Moreover, the long-term antihypertensive activity of rostafuroxin is
not associated with alterations of plasma potassium, RAAS, insulin resistance, plasma lipid
profile and uricemia. These findings indicate that the normalization of renal sodium
handling brought about by this compound is not accompanied by the typical side effects of
diuretics, such as: hypokaliemia, increased plasma levels of renin, aldosterone,
triglycerides and uric acid, or insulin resistance.
Increased levels of EO and the mutated adducin are both associated with the organ
complications related to hypertension, namely cardiac hypertrophy and progression toward
renal insufficiency. Cardiac and renal hypertrophy is induced in rats by chronic ouabain
infusion. Rostafuroxin prevents the ouabain-induced organ hypertrophy.
Rostafuroxin has shown a high safety ratio in toxicological studies and was well tolerated
in previous clinical trials.
Patients with mutated adducin and increased EO plasma levels share many functional, hormonal
and biochemical characteristics with MHS rats, therefore Rostafuroxin could become a first
choice treatment in such patients bearing specific gene mutations and presenting high
arterial blood pressure levels.
Preliminary proof of concept studies have shown ability of Rostafuroxin to reduce arterial
blood pressure levels in such a patients.
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Allocation: Randomized, Endpoint Classification: Efficacy Study, Intervention Model: Parallel Assignment, Masking: Double Blind (Subject, Caregiver, Investigator, Outcomes Assessor), Primary Purpose: Treatment
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