Journal of Lipid Research (Feb 2007)

Dynamics of dense electronegative low density lipoproteins and their preferential association with lipoprotein phospholipase A2

  • John W. Gaubatz,
  • Baiba K. Gillard,
  • John B. Massey,
  • Ron C. Hoogeveen,
  • Max Huang,
  • Eric E. Lloyd,
  • Joe L. Raya,
  • Chao-yuh Yang,
  • Henry J. Pownall

Journal volume & issue
Vol. 48, no. 2
pp. 348 – 357

Abstract

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Small, dense, electronegative low density lipoprotein [LDL(−)] is increased in patients with familial hypercholesterolemia and diabetes, populations at increased risk for coronary artery disease. It is present to a lesser extent in normolipidemic subjects. The mechanistic link between small, dense LDL(−) and atherogenesis is not known. To begin to address this, we studied the composition and dynamics of small, dense LDL(−) from normolipidemic subjects. NEFA levels, which correlate with triglyceride content, are quantitatively linked to LDL electronegativity. Oxidized LDL is not specific to small, dense LDL(−) or lipoprotein [a] (i.e., abnormal lipoprotein). Apolipoprotein C-III is excluded from the most abundant LDL (i.e., that of intermediate density: 1.034 < d < 1.050 g/ml) but associated with both small and large LDL(−). In contrast, lipoprotein-associated phospholipase A2 (LpPLA2) is highly enriched only in small, dense LDL(−). The association of LpPLA2 with LDL may occur through amphipathic helical domains that are displaced from the LDL surface by contraction of the neutral lipid core.

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