ESRD Clinical Trial
Official title:
Effect of N-Acetylcysteine on Peritoneal Membrane Function in Chronic Peritoneal Dialysis Patients.
The aim of our study is to investigate the effect of N-acetylcysteine on peritoneal small solute clearance and removal of salt and water in prevalent CAPD patients.
Cardiovascular disease is the commonest cause of morbidity and mortality in chronic dialysis
patients, including those treated with CAPD (Continuous Ambulatory Peritoneal Dialysis) [1].
Uncontrolled arterial hypertension in ESRF leads to progression of LVH, which is a strong
predictor for coronary events, CHF and mortality [2]. Fluid overload is a major factor in
the pathogenesis of arterial hypertension in CAPD patients [3]. Therefore, interventions to
optimize volume status, and hence blood pressure, are considered central in the management
of such patients. Such therapies include restricting dietary sodium and water intake, use of
diuretics in patients with residual renal function and optimization of peritoneal
ultrafiltration with sodium and water removal [1]. As shown in the EAPOS Study, peritoneal
ultrafiltration was important predictor of mortality [4].
Peritoneal fluid and salt removal can be increased by using a more hypertonic dialysis fluid
using glucose as osmotic agent. Consistent use of hypertonic glucose solutions may damage
peritoneal membrane and may also lead to increased systemic absorption of glucose with
subsequent hyperglycemia, increased thirst and excessive water drinking. Concerns about the
role of glucose in deterioration of peritoneal membrane function have been supported in
recent studies [5]. Generally, the evolution of peritoneal membrane properties over time is
characterized by a progressive increase in small solute transport, leading to higher glucose
absorption rate from peritoneal fluid and loss of ultrafiltration capacity [6]. Such a high
peritoneal transport status is associated with less peritoneal fluid removal, overhydration,
hypertension and LVH. High peritoneal transport status is a risk factor of mortality in CAPD
patients [7].
In recent years, there has been an increasing focus on association between inflammation,
increased oxidative stress and high peritoneal transport rate and their relation to
mortality in CAPD patients [8 ]. Inflammation has been shown to increase a peritoneal
transport rate in CAPD patients [8]. Both inflammation and increased oxidative stress may
impact to inadequate fluid removal. The exact mechanism of this phenomenon is not fully
understood.
Several experimental and clinical studies showed that increased oxidative stress in dialysis
patients may be due to inhibition of nitric oxide (NO) synthesis by ADMA (Asymmetric
Dimethylarginine ), known to be endogenous inhibitor of NO synthetase [9]. ADMA may be
significantly reduced by dialysis [10]. Metabolism of ADMA is primarily by the enzyme DDAH ,
which activity is decreased by inflammation, oxidative stress, diabetes mellitus and
hypercholesterolemia [11]. It was proposed that circulating ADMA may be one mechanism
accounting for the resistant hypertension and fluid overload in dialysis patients [11].
Based on current knowledge, treatment aimed at reducing oxidative stress should decrease
ADMA levels [11], and it is logical to suggest that such a therapy might improve BP control
and fluid status in CAPD patients. In our opinion, it is worth to check an ability of
antioxidant therapy to produce a favorable effect on biological properties of peritoneal
membrane. One preliminary study on effect of antioxidant Vitamin E showed a small beneficial
effect on ADMA in chronic kidney disease [12].
N-Acetylcysteine (NAC) is an active antioxidant proved to be safe and beneficial in
hemodialysis patents [13]. In our recent study, NAC effectively reduced the ototoxic effect
of gentamicin in chronic hemodialysis patients [14].
The aim of our study is to investigate the effect of N-acetylcysteine on peritoneal small
solute clearance and removal of salt and water in prevalent CAPD patients.
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Allocation: Non-Randomized, Endpoint Classification: Bio-equivalence Study, Intervention Model: Single Group Assignment, Masking: Open Label, Primary Purpose: Treatment
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