Hypertension Clinical Trial
Official title:
A Study Looking at the Effects of a Modest Reduction in Dietary Salt Intake on Blood Pressure Control in Haemodialysis Patients
High blood pressure (hypertension) affects up to 80% of all patients receiving haemodialysis
for chronic kidney disease (CKD). High blood pressure is a major cause cardiovascular
disease (i.e. strokes, heart attacks and heart failure) and, thereby, cardiovascular deaths
in these patients.
A significant cause of raised blood pressure in haemodialysis patients is thought to be due
to retention of salt in the body. In healthy people the kidneys excrete salt but the kidneys
of patients with CKD cannot do this, so salt has to be removed by dialysis. However dialysis
cannot remove as much salt as is necessary, and so it accumulates. This fact has been
recognized for many years, and health professionals caring for haemodialysis patients often
stress the importance of restriction of dietary salt intake.
However no research has looked in detail at the mechanisms by which salt raises blood
pressure in haemodialysis patients. It is likely that salt directly affects thirst, causing
patients to drink more and become overloaded with fluid. In addition, salt may have direct
effects on the blood vessel wall, causing failure of adequate blood vessel relaxation. Both
of these factors may raise blood pressure.
We will conduct a carefully controlled crossover study looking at the effects of a modest
reduction in salt intake on BP. During the course of the study, which will last eight weeks,
patients will receive both a 5 gram per day and a 10 gram per day salt intake. We will look
at how thirst, fluid intake, a number of markers of blood vessel function and blood pressure
differ on these two salt intakes.
High blood pressure (BP) is a major independent risk factor for cardiovascular mortality in
individuals on haemodialysis, and yet BP is extremely poorly controlled in this population.
Excessive dietary salt intake is likely to be a major cause of hypertension in these
patients. Firstly, excessive salt intake will result in thirst, excessive fluid intake and
weight gains between dialysis, and thereby chronic over-expansion of extracellular fluid
volumes resulting in high blood pressure. Secondly, salt may have direct effects on the
arterial tree contributing to endothelial dysfunction that has clearly been demonstrated in
uraemic individuals, including haemodialysis patients. Abnormalities in endothelial nitric
oxide (NO) production may play an important role in salt-sensitive hypertension, mediated by
the potent inhibitor of NO synthase, asymmetrical dimethylarginine (ADMA). Plasma ADMA
concentrations are several-fold higher in individuals on dialysis than in normal controls,
and it would be of interest to see whether ADMA concentrations decrease with a reduction
dietary salt intake.
In spite of the importance of dietary salt intake in haemodialysis patients, there are no
controlled studies which delineate the mechanisms by which salt intake affects BP. We
propose to conduct a prospective double-blind placebo controlled cross-over study of normal
(10 to 12 grams salt per day) versus modestly reduced (6 grams per day) salt intake over an
eight week period in haemodialysis patients. The primary outcome measure is the change in
pre-dialysis systolic BP. Other outcome measures include mean systolic and diastolic BP as
measured by ABPM, thirst scores, daily weight gains and thoracic fluid content, as measured
by thoracic bioimpedance. Furthermore, in a sub-group of subjects will we study the changes
in plasma ADMA concentrations with reductions in salt intake, and examine correlations with
changes in BP and systemic vascular resistance.
;
Allocation: Randomized, Endpoint Classification: Safety/Efficacy Study, Intervention Model: Crossover Assignment, Masking: Double-Blind, Primary Purpose: Treatment
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