Title of article
Role of the macrophage galactose lectin in the uptake of desialylated LDL
Author/Authors
Anna L. Bartlett، نويسنده , , Thomas Grewal، نويسنده , , Elena De Angelis، نويسنده , , Simon Myers، نويسنده , , Keith K. Stanley، نويسنده ,
Issue Information
روزنامه با شماره پیاپی سال 2000
Pages
12
From page
219
To page
230
Abstract
Desialylated low density lipoprotein (LDL) is rapidly taken up and accumulated by both peripheral blood monocytes and cells isolated from human arterial intima consisting predominantly of smooth muscle cells. It is shown that thioglycollate (TG)-elicited mouse macrophages and mouse peritoneal macrophages stimulated with lipopolysaccharide (LPS) show increased expression of a membrane-bound, galactose-specific lectin that could be responsible for this uptake. In LPS-stimulated macrophages accumulation of desialylated LDL is increased ca. 2.6-fold. Accumulation of acetylated LDL in the same cells is reduced, suggesting that the galactose-specific lectin might be responsible for the uptake of desialylated LDL. Transfection of cells with the mouse macrophage Gal/GalNAc-specific lectin (MMGL) increased their capacity to take up asialofetuin (ASF) and, to a smaller extent, desialylated LDL. The uptake of desialylated LDL was small, most likely due to the high kd of MMGL for biantennary oligosaccharides as found on LDL, and low concentration of LDL achieved in tissue culture experiments. The data suggest that the expression of galactose-specific lectins can be elevated under inflammatory conditions, and that these receptors could contribute to foam cell formation under conditions of high desialylated LDL concentration, as might be found in arterial intima.
Keywords
Lipopolysaccharide , MMGL , scavenger receptor , Desialylated LDL , lectin
Journal title
Atherosclerosis
Serial Year
2000
Journal title
Atherosclerosis
Record number
630137
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