Renal Insufficiency, Chronic Clinical Trial
Official title:
A Double Blind Clinical Trial to Examine the Renal Effects of an Angiotensin Converting Enzyme Inhibitor (Enalapril) in Adults With Chronic Kidney Disease of Uncertain Aetiology (CKDu)
Enalapril would significantly reduce progression of renal disease in patients with Chronic Kidney Disease of Uncertain aetiology.
End Stage Kidney Disease (ESKD) results in reduced life expectancy, quality of life and
increased consumption of health care resources. Chronic Kidney Disease of Uncertain
aetiology (CKDu) is being increasingly recognized in the North Central Region of Sri Lanka
and in certain regions over 25% (unpublished data) of general population is suspected as
suffering from CKDu. The number of patients who reach ESKD that requires hemodialysis or
transplantation is increasing, highlighting the need to find strategies that slow
progression of kidney disease. The need for these strategies is even more critical in Sri
Lanka where dialysis in not a preferred treatment option. Treatment strategies should be
readily accessible and cheap.
The importance of proteinuria as a significant risk factor for ESKD is well recognized, and
treatment that is targeted at reducing proteinuria has been shown to reduce progression of
renal disease. The Renin - Angiotensin - Aldosterone - System (RAAS) is directly involved in
the regulation of blood pressure, fluid volume, and vascular response to injury and
inflammation. The inappropriate activation of this system causes hypertension, fluid
retention, and inflammatory, thrombotic, and atherogenic effects that may contribute to
end-organ damage in the long term. Angiotensin II mediates hemodynamic effects as well as
inflammation and fibrosis in the kidney, heart, and vasculature.
Numerous clinical trials have established that interruption of the RAAS cascade with
angiotensin-converting enzyme inhibitors (ACEI) or angiotensin receptor blockers (ARB) is
beneficial in slowing progression of renal disease. Reduction of BP lowers proteinuria, but
the use of an ACEI or an ARB reduces both proteinuria and the rate of deterioration of renal
function beyond those seen with equivalent BP reduction from conventional antihypertensive
agents. However, the use of these agents has limitations, with significant numbers of
treated patients still demonstrating progressive renal disease. RAAS blockers have been
shown to blunt the progression of advanced kidney disease. However the long-term renal
effect of these agents in early renal disease is not well demonstrated. In fact the trials
which showed benefits with RAAS blockers did show in glomerular disease and evidence is not
so strong in tubulo-interstitial disease. The benefits of RAS inhibition seem to depend on
the degree of proteinuria at baseline. It is marginal in those with low grade proteinuria.
In most forms of proteinuric chronic renal disease, glomerular filtration rate continues to
decline even when the initial insult has been removed. The cause of CKDu is still unknown.
CKDu is a tubulo-interstitial disease with low grade proteinuria. We believe that the place
of ACEI for secondary prevention of CKDu progression needs investigation
;
Allocation: Randomized, Endpoint Classification: Efficacy Study, Intervention Model: Parallel Assignment, Masking: Double Blind (Subject, Caregiver, Investigator, Outcomes Assessor), Primary Purpose: Treatment
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