Hypertension Clinical Trial
Official title:
An Open-label PET-observer-blinded Pilot Study of the Effect of Aliskiren- Versus Amlodipine-based Antihypertensive Treatment in Patients With Small Abdominal Aortic Aneurysm and Mild to Moderate Hypertension on Aneurysmal FDG-uptake
Inflammation of the blood vessel plays an important role in the development and growth of a dilated abdominal aorta. An elevated blood pressure leads to an increase in inflammation, therefore blood pressure lowering is an important part of the treatment of patients with a dilated abdominal aorta who also have an elevated blood pressure. In the investigators study the investigators compare the anti-inflammatory effects of 2 different blood pressure lowering strategies. The investigators hypothesize that both strategies will decrease inflammation, however the investigators believe the total decrease of inflammation depends on the type of blood pressure lowering medication used.
Standard therapy of small AAAs currently consists of "watchful waiting" strategy with
aggressive blood pressure control "Watchful waiting" includes an Ultrasound (more recently
CT or MRI scan) every 12 months (for AAAs between 3.5 - 4.4 cm) or every 6 months (for AAAs
between 4.5 and 5.5 cm) to observe. A growth rate of >7 mm/ 6 months has been suggested as a
threshold for proceeding to aneurysm repair irrespective of aneurysm size. Clearly, there is
need for a more sensitive method to evaluate the progress of AAA growth.
Recent publications have shown that evaluation of AAAs using FDG-uptake with PET-scan may
identify small AAAs that are more prone to grow and/or rupture, as these AAAs as compared to
normal aorta's show increased inflammatory activity , which is considered the major
pathophysiological pathway. Evaluation of FDG-uptake is also sensitive enough to observe the
short-term effects of endovascular intervention of large AAAs, as unpublished data show a
statistically significant reduction in aneurismal FDG-uptake only 6 weeks after endovascular
repair of large AAAs. Therefore, the change in aneurismal FDG-uptake may also be a very
promising and sensitive method to evaluate treatment effects of medical interventions within
a relatively short period of time (3 months).
Just as pressure unloading may represent an anti-inflammatory mechanism in endovascular
repair of more advanced aneurysms, so may milder pressure unloading in moderately
hypertensive individuals with smaller aneurysms display similar anti-inflammatory effects.
Such a mild form of pressure unloading may be attainable with adequate anti-hypertensive
drug therapy. In this context, however, a possible additional benefit may be that some
anti-hypertensive drug classes have been proposed to exert specific anti-inflammatory
effects relevant to aneurysm inflammation.
Local activation of multiple components of the renin angiotensin system has been implicated
in both the development of aneurysms, as well as in their inflammatory component. In
accordance, preliminary evidence from murine studies suggest that ACE inhibitors, for
example, may reduce inflammatory activity in aneurysmatic vessel walls. However, since ACE
inhibitors block the renin angiotensin system halfway it's path, and non-ACE conversion of
angiotensin I occurs, a rationale exists to block the renin angiotensin system upstream of
ACE. Upstream blockade of the renin-angiotensin system may have additional advantages in
antagonising direct pro-inflammatory effects of renin itself, which have been identified in,
for example, kidney tissue and retinal microvessels.
A case can thus be made for renin inhibition as a potential optimal strategy for reducing
aneurysm inflammation in hypertensive patients with aortic aneurysms. In the proposed pilot
trial, the direct renin inhibitor Aliskiren will be evaluated. As a control condition, an
antihypertensive agent without postulated specific anti-inflammatory effects is appropriate.
Calcium channel blockers represent such a class.
The current study will explore what the size and variability of the effect of aliskiren
monotherapy, the combination of aliskiren/hydrochlorothiazide, amlodipine monotherapy, or
the combination of amlodipine/hydrochlorothiazide on FDG-uptake is (if at all measurable on
top of the effect of antihypertensive and statin therapy). This will allow more accurate
power calculation of larger future studies aiming at prevention of AAA-progression (diameter
and rupture).
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Allocation: Randomized, Intervention Model: Parallel Assignment, Masking: Open Label, Primary Purpose: Treatment
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