lipid mgmt in ckd
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Lipid Management in Chronic Kidney Disease Patients
Tejas Desai, MDECU Nephrology & Hypertension
Office: 252-744-2113Email: desait@ecu.edu
Version 1: 9/17/9
Historical Controversies
• Known that for every Δ -40 mg/dL of total cholesterol in patients with pre-existing CAD & without CKD per se, there is a Δ -25-30% risk of MI or CVA
• Most of these trials did not focus on CKD patients– Some have even excluded CKD patients from their
investigations altogether
Proceedings of the Royal College of Physicians 1999, Volume 29, pp. 10-15Lancet 2002, Volume 360, pp. 7-22NEJM 2000, Volume 343, pp. 317-326Diabetes Care 1993, Volume 16, pp. 434-444
Historical Controversies
• Some have argued that lipid-lowering therapy in CKD and ESRD patients may be harmful if drug effects are not studied first
• Some have argued that only 25% of deaths in CKD/ESRD patients are due to MI (75% due to congestive heart failure, arrhythmias, sudden cardiac death)– Conditions that are not easily treated with lipid-
lowering agents
Intuitively, it makes sense to treat CKD patients with Lipid-lowering agents
• All CKD/ESRD patients are at increased risk for vascular disease
• Lipid-lowering agents, such as statins, have shown a benefit in halting the progression of atherosclerotic vascular disease in non-CKD patients– Why would we not see a similar beneficial effect in
CKD/ESRD patients?• SHARP Trial
SHARP
• Study of Heart and Renal Protection• A trial designed to look for any benefits of
lipid-lowering agents in patients with CKD/ESRD
• Prefaced by 2 pilot studies to assess safety of statins in CKD patients– UK-HARP I and UK-HARP II
UK-HARP I
• Goals– Assess biochemical efficacy & safety of simvastatin
20 mg daily in CKD patients for 1 year– Establish the feasibility of conducting a large-scale
randomized control trial
*Note: also assessed the safety of 100 mg of ASA daily in CKD patients for 1 year
American Journal of Kidney Diseases, 2005, Volume 45, Issue 3.
UK-HARP I
• Inclusion Criteria– Anyone > 18 years
of age– CKD: Cr > 1.7 mg/dl– HD or PD patients– PCP or Nephrologist
found no compelling reason to start a statin or a contraindication to one
American Journal of Kidney Diseases, 2005, Volume 45, Issue 3.
• Exclusion Criteria– If the MD felt statin
therapy was required
– h/o inflammatory muscle disorders, uremia recently, or liver disease
UK-HARP I: American Journal of Kidney Diseases, 2005, Volume 45, Issue 3.
UK-HARP I: American Journal of Kidney Diseases, 2005, Volume 45, Issue 3.
Thus far…
• UK-HARP I– 20 mg/d simvastatin leads to sustained decreases
in LDL, total cholesterol– No major differences in side effects
• UK-HARP II– “a little more greedy”– Can the addition of ezetimibe to 20 mg/d
simvastatin lead to even greater reductions in cholesterol in CKD patients?
UK-HARP II
• Inclusion & Exclusion criteria were the same as in UK-HARP I
American Journal of Kidney Diseases, 2006, Volume 47, Issue 3, pp. 385-95
UK-HARP II: American Journal of Kidney Diseases, 2006, Volume 47, Issue 3, pp. 385-95
UK-HARP II: American Journal of Kidney Diseases, 2006, Volume 47, Issue 3, pp. 385-95
Summary of UK-HARP I & II
SHARP
• Aim is to study 3000 dialysis patients & 6000 CKD patients
• Assess whether lipid-lowering agents can retard the progression of CKD and time to dialysis
• Results not available as of today
What evidence does exist as of today?
• GREACE Study: Treatment of dyslipidemias in patients with CAD– Not on statin: 5.2% decrease in CrCl– On a statin: 4.9 – 12% increase in CrCl
• Pravastatin Pooling Project (PPP): Treatment of dyslipidemias in patients with CKD at risk for CAD– Pravastatin decreased the risk for MI, surgical revascularization, or coronary death in
moderate CKD patients (HR 0.77, p < 0.05)
• Meta-Analysis looking at statins and their effects on renal outcomes– Modest improvement in proteinuria (-0.37g/24h) & albuminuria (-0.02g/24h)– Modest improvement in halting progression of kidney function (1.22 ml/min/yr slower
than placebo)
Journal of Clinical Pathology, 2004, Vol. 57, pp. 728-734Circulation, 2004, Vol. 10, pp. 1557-63JASN, 2006, Vol. 17, pp. 2006-2016
Summary
• UK-HARP I & II have set the stage for a large, RCT to determine if statins +/- ezetimibe can retard kidney failure
• SHARP is the trial that we are awaiting for definitive guidance
• Until then, UK-HARP I & II, along with the previous studies, suggest that we should initiate statin therapy to at least lower the risk of CAD, coronary death, and need for surgical revascularization
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