CHANGES IN SERUM LIPOPROTEIN(A) IN HYPERLIPIDEMIC SUBJECTS UNDERGOINGLONG-TERM TREATMENT WITH LIPID-LOWERING DRUGS

Though the exact physiology and pathology of lipoprotein (a) [Lp(a)] r emains unknown, it has been demonstrated that increased serum Lp(a) le vels are correlated with an increased risk of atherosclerotic vascular disease. The effects of lipid-lowering drugs on Lp(a) levels is uncle ar because of inconsistencies between study designs, This study analyz es the effects of the commonly used lipid-lowering drugs pravastatin ( PRAV), lovastatin (LOV), and cholestyramine (CIIOL) on serum Lp(a) and other serum lipid levels in a parallel study design. Hyperlipidemic m en (n = 32) were enrolled from three centers and treated for 48 weeks in a multicenter clinical trial using PRAV, LOV, CIIOL, or a placebo ( for the first 16 weeks only), Baseline serum low-density lipoproteins (LDL-C), high density lipoproteins (HDL-C), and triglycerides were 199 +/- 38, 40 + 9, and 160 +/- 70 mg/dl, respectively. At the end of 48 weeks, serum plasma LDL-C declined in patients randomized to PRAV, LOV , and CHOL, respectively, by 31%, 29%, and 23% (all p < 0.001); HDL in creased by 4%, 11%, and 11% (all p < 0.001); and TG changed by -16%, - 28%, and +43% (all p < 0.001). Subjects in PRAV and LOV changed Lp(a) by 9% and 3%, respectively. Although there was an initial Lp(a) declin e in the first 8 weeks of CHOL therapy (p < 0.05, ANOVA), this returne d-to baseline after 48 weeks. In this parallel study design PRAV, LOV, and CHOL are effective LDL-lowering medications with minimal effects on plasma p(a).