Hypertension Clinical Trial
Official title:
The Effect of Moxonidine and Regression of Early Target Organ Damage in Young Subjects With Abdominal Obesity and Hypertension: a Randomised, Double Blind, Active Comparator Clinical Trial
Obesity is a major risk factor for the development of hypertension. Based on population
studies, risk estimates indicate that at least two-thirds of the prevalence of hypertension
can be directly attributed to obesity. Obesity per se is commonly associated with activation
of the sympathetic nervous system with a predominant increase in sympathetic outflow to the
kidneys and the peripheral vasculature and there is now conclusive evidence that heightened
sympathetic nerve activity is a major contributor to the elevation in blood pressure
associated with obesity, particularly in young subjects. In line with these findings,
dietary weight loss has repeatedly been demonstrated to result in reduced sympathetic nerve
activity and lower blood pressure levels.
Several lines of evidence have well documented the significant role of SNS activation in
obesity associated hypertension and target organ damage. Weight loss is the preferred
treatment option for obesity and its consequences and reduces both SNS activation and blood
pressure. In the real world however, weight loss maintenance is rarely achieved in obese
patients highlighting the urgent need for alternative treatment strategies. Given the
crucial involvement of SNS activation in various aspects of the obesity related increase in
blood pressure, target organ damage and cardiovascular risk, the use of sympatho-inhibitory
agents at an early stage is an obvious choice.
The investigators therefore plan to examine the effects of the centrally sympatholytic agent
moxonidine on blood pressure and the morning surge in blood pressure, sympathetic activity,
regression of early target organ damage (heart, kidney and endothelium), metabolic and
inflammatory markers in young obese subjects with hypertension in a randomized, double-blind
clinical trial with the angiotensin receptor blocker irbesartan as an active comparator to
achieve similar blood pressure reductions in both groups. The investigators hypothesize that
moxonidine treatment will result in significant improvements in these outcome parameters and
beneficial effects beyond simple blood pressure reduction.
Findings from this study could pave the way for an early and pathophysiology- tailored
treatment strategy of obesity related hypertension and its detrimental consequences.
n/a
Allocation: Randomized, Endpoint Classification: Efficacy Study, Intervention Model: Parallel Assignment, Masking: Double Blind (Subject, Caregiver, Investigator), Primary Purpose: Treatment
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