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Treatment and prognosis of IgA nephropathy page-4
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Controlled trials of Fish Oil


Randomized controlled trials evaluating fish oil in patients with IgA nephropathy have reported conflicting results [58-64] . The following two trials illustrate the range of findings [58,61,64] :
In a trial from the Mayo Clinic, 106 patients with baseline creatinine clearance 80 mL/min and protein excretion of 2.5 to 3 g/day were randomly assigned to therapy with either 12 g of omega-3 fish oil or a similar amount of olive oil for two years [58] . There was no difference in blood pressure control and no effect on protein excretion during the study.



It is not clear why these trials produced different results. One potentially important factor is that the positive trial evaluated patients with more advanced disease (more proteinuria and lower creatinine clearance at baseline), and the placebo (olive oil) group had a faster rate of progression than is generally seen. On the other hand, in the negative trial, patients in the placebo group had lower baseline proteinuria, a factor that is known to be associated with a better prognosis [64] .


A meta-analysis evaluating five controlled trials, which was published before the negative findings from the Southwest Pediatric Nephrology Study Group, attributed much of the variability in the reported results to differences in the duration of follow-up [65] . When this difference was accounted for statistically, a benefit with fish oil therapy was not found to be significant, but a minor benefit was possible.
Summary — The benefit of fish oil has not been established. Furthermore, the trial designs are not applicable to current practice, since the patients were not treated with an ACE inhibitor and/or ARB and, as necessary, other drugs to recommended proteinuria and blood pressure goals. (See "Treatment goals" above and see "Antihypertensive therapy and progression of nondiabetic chronic kidney disease").
Fish oil can be tried in addition to ACE inhibitors and/or ARBs in patients with protein excretion >500 to 1000 mg/day, a gradual reduction in GFR, and mild to moderate histologic lesions [66] .


Lipid-lowering therapy — All patients with decreased kidney function and/or hypercholesterolemia should receive lipid-lowering therapy with a statin based upon the following rationales:
Chronic kidney disease is associated with a marked increase in cardiovascular risk, and is now considered a coronary artery disease risk equivalent. (See "Chronic kidney disease and coronary heart disease").
Lipid-lowering with statins has been associated with a slower rate of loss of glomerular filtration rate in patients with mild to moderate CKD. (See "Statins and chronic kidney disease", section on Statins and CKD progression.
The goal LDL-cholesterol is similar to that in patients with underlying coronary heart disease. (See "Intensity of lipid lowering therapy in secondary prevention of coronary heart disease"). There is a risk of Rhabdomyolysis, one of the most dangerous Zocor side effects, may be reversible once patients stop taking the popular anti-cholesterol drug.  Zocor rhabdomyolysis is serious form of muscle injury which causes muscle cells and fibers to enter the bloodstream. The condition can induce compromised kidney function and even cause death for certain individuals.  However, for some patients, merely discontinuing treatment with Zocor can reverse the degenerative process as muscles heal.

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