LIPOPROTEIN(A) AS A RISK FACTOR FOR PRECLINICAL ATHEROSCLEROTIC DISEASE IN A BIRACIAL COHORT - THE ATHEROSCLEROSIS RISK IN COMMUNITIES (ARIC) STUDY

Lipoprotein(a) (Lp(a)) is a risk factor for clinically manifest coronary heart disease (CHD) and cerebrovascular disease in Caucasian and in Asian populations. The role of Lp(a) as a risk factor in blacks has not been described, despite the markedly higher levels of Lp(a) and excess CHD and stroke prevalence observed in middle-aged blacks compared with whites. Further, little information exists on the association of Lp(a) and asymptomatic atherosclerosis in any race or gender group. In this report, 15 700 middle-aged black and white participants in the Atherosclerosis Risk in Communities (ARIC) Study had complete B-mode ultrasound scans of their extracranial carotid arteries. Of the 13 384 individuals with complete B-mode data at the carotid bifurcation, those with mean carotid bifurcation ;intima-media wall thicknesses at or above the 90th percentile of the population distribution (similar to 1.2 mm) were considered to have carotid atherosclerosis. Lp(a) was measured as its total protein content by double-antibody ELISA for apo(a) detection. Blacks in this study had mean Lp(a) protein values that were twice as high as those of whites (168.9, 147.1, 86.6, and 75.1 mu g/ml for black females, black males, white females, and white males, respectively). For all race and gender groups, Lp(a) protein concentrations were higher among individuals with carotid atherosclerosis than for those without. From these cross-sectional data, we conclude that Lp(a) protein is a risk factor for preclinical atherosclerosis as well as for clinically manifest cardiovascular disease. The high Lp(a) levels in blacks, without correspondingly thickened intima-media walls at the carotid bifurcation, suggest that race and gender differences in apo(a) phenotypes, hemostatic activity, or other unrelated risk factors may contribute to this paradox.