Lipoprotein(a) and Atherosclerosis

doi:10.1059/0003-4819-115-3-209

Lipoprotein(a) and Atherosclerosis

Angelo M. Scanu, MD;
Richard M. Lawn, PhD; and
Kåre Berg, MD, PhD

Abstract

▪Lipoprotein(a) [Lp(a)], a lipoprotein variant, was relegated for almost 25 years to the study of a few specialists. During the past 3 to 4 years, however, there has been a tremendous upsurge of interest in Lp(a), primarily because of multidisciplinary efforts in structural and molecular biology. Findings emerging from these efforts include the following: Lp(a) represents a cholesteryl-ester, low-density-lipoprotein (LDL)-like particle with apolipoprotein (apo) B-100 linked to apo(a); apo(a) is a glycoprotein coded by a single gene locus on the long arm of chromosome 6, which has several alleles, accounting for its remarkable size polymorphism (300 to 800 kD); apo(a) size polymorphism relates to plasma levels and density distribution of Lp(a); apo(a) is strikingly similar to plasminogen; and in vitro, Lp(a), in appropriate levels, competes for some physiologic functions of plasminogen in the coagulation and fibrinolytic cascade and may thus be thrombogenic. The LDL-like properties of Lp(a) may also confer atherogenic potential, but the mechanisms underlying this atherogenicity remain to be defined. In epidemiologic studies, high plasma Lp(a) levels have been associated with an increased incidence of atherosclerotic cardiovascular disease, especially in patients less than 60 years of age. Moreover, Lp(a) has been found as an intact particle in the arterial intima, particularly in association with atherosclerotic plaque. This finding suggests that Lp(a) can traverse the endothelium, possibly by a non-receptor-mediated process, and, at the intimal level, acquire thrombogenic and atherogenic potentials. Current information justifies the need to determine plasma Lp(a) levels in patients with a history of atherosclerotic cardiovascular disease. Unfortunately, the available techniques need to be standardized. Apolipoprotein(a) exists in isoforms of different sizes, and the importance of determining apo(a) phenotypes in clinical practice remains to be established.

Article and Author Information

An edited summary of an Interdepartmental Dean's Conference arranged by the Department of Medicine of the University of California, Davis, School of Medicine, Davis, California, and the Department of Veterans Affairs Martinez Medical Center, Martinez, California, and held on 16 May 1990. Michael C. Geokas, MD, PhD, is permanent chairman and organizer of these conferences.
Authors who wish to cite a section of the conference and specifically indicate its author can use this example for the form of reference:

Lawn RM. The structure and evolution of apolipoprotein(a), pp 209-211. In: Scanu AM, moderator. Lipoprotein(a) and atherosclerosis. Ann Intern Med. 1991;115:209-218.
Grant Support: In part by Genentech, Inc. (Dr. Lawn); by the Norwegian Council on Cardiovascular Disease (Dr. Berg); and by Program Project NIH-NHLBI 18577 (Dr. Scanu and colleagues).
Requests for Reprints: Michael C. Geokas, MD, PhD, 106 Castle Crest Road, Walnut Creek, CA 94595.
Current Author Addresses: Dr. Lawn: Division of Cardiovascular Medicine, Stanford University School of Medicine, Stanford, CA 94305-5246.

Dr. Berg: Institute of Medical Genetics, University of Oslo, and Department of Medical Genetics, Ullevål Hospital (Oslo City Hospital), P. O. Box 1036, Blindem, 0315 Oslo 3, Norway.

Dr. Scanu: Departments of Medicine, Biochemistry, and Molecular Biology, University of Chicago, Chicago, IL 60637.