End Stage Renal Disease Clinical Trial
Official title:
Effect of Add-on Spironolactone to Losartan Versus Losartan Alone on Peritoneal Membrane Among Continuous Ambulatory Peritoneal Dialysis Patients: An Open-Label Randomized-Controlled Trial
The ESCAPE-PD (Effects of add-on SpironolaCtone to losartan versus Alone on Peritoneal mEmbrane among continuous ambulatory Peritoneal Dialysis patients) study is a randomized, open-label, single center, active-controlled clinical trial. Adults end-stage kidney disease patients 18 years or older undergoing continuous ambulatory peritoneal dialysis (CAPD) will be enrolled. A total 84 CAPD will be randomly assigned to either the combination of spironolactone and losartan (experimental arm) or losartan alone (control arm). The primary outcomes are the difference in peritoneal dialysate effluent cancer antigen-125 (CA-125) and peritoneal equilibration test (PET) indices (dialysate-to-plasma creatinine ratio, 4-hour ultrafiltration volume, and the concentration of glucose present in the solution at the start of the test). Secondary outcome measures include laboratory and mechanistic outcome measures, nutrition outcomes, health-related quality of life, physical function, clinical events, and safety profiles. Results will be disseminated to suggest a strategy to prevent the peritoneal membrane function among CAPD patients through peer-reviewed publications along with scientific meetings.
Peritoneal dialysis (PD) is one of the methods of renal replacement therapy (RRT) that can
easily perform at home. The declared "PD first" policy from the National Health Security
Office causes rapidly expansion of this group of patients. In the year 2013, the current
study in Thailand showed that the patients enrolled for peritoneal dialysis accumulated for
more than 15,000 people. It works continuously similar to the actual function of the kidneys
in normal people. In addition, PD also helps to slow the decline of remaining kidney function
(residual renal function), which is very important and affect in decreasing mortality rate in
this group of patients. However, PD has several limitations such as complications from the
infection and high failure rate associated with a dysfunction of the peritoneal membrane
during long-term treatment. Approximately 4-12 percent of patients will have ultrafiltration
failure and volume overload in the first couple of years of treatment and soar to 30-50
percent in patients treated for more than six years.
The causes of peritoneal membrane deterioration are exposure to incompatible dialysis
solution with hyperosmolar glucose content, acidic pH, reactions to PD catheter material,
uremia and peritonitis. The alterations of structural and functional of the peritoneal
membrane after exposed to these several insults are epithelial-to-mesenchymal transition
(EMT), and increase in peritoneal solute transport, which consequently leading to peritoneal
dialysis failure. It has been already demonstrated that the local
renin-angiotensin-aldosterone system (RAAS) plays a key role in this regulation by promoting
the activation of neoangiogenesis and fibrotic pathways.
According to the pathophysiologic changes of the peritoneal membrane, Angiotensin Converting
Enzyme Inhibitors (ACEIs) and Angiotensin Receptor Blockers (ARBs) are adapted to be use in
respect of membrane preserving agents. Many studies, both in human and animal models,
demonstrate the protective effect against peritoneal membrane deterioration by inhibiting the
formation of transforming growth factor beta1 (TGF-β1), vascular endothelial growth factor
(VEGF), and decreasing progression rate of small to high transport membrane type. In fact,
mineralocorticoid receptor antagonists (MRAs) seem to have higher efficacy than ACEIs/ARBs in
some experimental models. The possible mechanism is the effects of mineralocorticoid receptor
antagonists that not only inhibit the formation of TGF- β1 and VEGF, but also suppress
intracellular Reactive Oxygen Species (ROS) generation, activation of extracellular
signal-regulated kinase (ERK) 1/2, and p38 mitogen-activated protein kinase (MAPK), the
substrates responsible for aldosterone induces alterations in cell phenotype. A prospective
cohort study of 23 CAPD patients was conducted and evaluated the effect of spironolactone on
peritoneal membrane. The result showed the possible benefit of spironolactone in slowing the
decline of peritoneal function, suppressing the elevation of profibrotic markers, and
increasing mesothelial cell mass.
As a result of the clinical practice, most of CAPD patients tend to receive ACEIs/ARBs as
prescribe by the clinicians, in order to control blood pressure, raise serum potassium level,
and others compelling indications. Thus, the concept of add-on MRAs to ACEIs/ARBs, desiring
the synergistic effects of these 2 drugs group, for membrane preservation is challenge.
Notwithstanding the fact that current evidence about the combination effects of ACEIs/ARBs
with MRAs is limited in term of quality of the study, sample size, inadequate follow-up
period, and poor sensitive parameter in assessing the structural and functional changes of
the peritoneal membrane. Thereby, this study aims to evaluate the effect of add-on
spironolactone to losartan versus losartan alone on membrane preservation in continuous
ambulatory peritoneal dialysis patients.
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