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J Biol Chem, Vol. 275, Issue 3, 1635-1644, January 21, 2000
From the Cell Biology Group, The Heart Research Institute,
Camperdown, New South Wales 2050, Australia
Murine and human macrophages rapidly decreased
the level of cholesteryl ester hydroperoxides in low density
lipoprotein (LDL) when cultured in media non-permissive for LDL
oxidation. This process was proportional to cell number but could not
be attributed to the net lipoprotein uptake. Macrophage-mediated loss
of lipid hydroperoxides in LDL appears to be metal ion-independent.
Degradation of cholesteryl linoleate hydroperoxides was accompanied by
accumulation of the corresponding hydroxide as the major product and
cholesteryl keto-octadecadienoate as a minor product, although taken
together these products could not completely account for the
hydroperoxide consumption. Cell-conditioned medium possessed a similar
capacity to remove lipid hydroperoxides as seen with cellular
monolayers, suggesting that the activity is not an integral component
of the cell but is secreted from it. The activity of cell-conditioned medium to lower the level of LDL lipid hydroperoxides is associated with its high molecular weight fraction and is modulated by the availability of free thiol groups. Cell-mediated loss of LDL
cholesteryl ester hydroperoxides is facilitated by the presence of
Macrophages Can Decrease the Level of Cholesteryl Ester
Hydroperoxides in Low Density Lipoprotein*
,
-tocopherol in the lipoprotein. Together with our earlier reports on
the ability of macrophages to remove peroxides rapidly from oxidized
amino acids, peptides, and proteins as well as to clear selectively cholesterol 7-
-hydroperoxide, results presented in this paper provide evidence of a potential protective activity of the cell against
further LDL oxidation by removing reactive peroxide groups in the lipoprotein.
*
This work was supported by Grant 980298 from Australian
National Health and Medical Research Council (to W. J.).The costs of publication of this
article were defrayed in part by the
payment of page charges. The article
must therefore be hereby marked
"advertisement" in
accordance with 18 U.S.C. Section
1734 solely to indicate this fact.
To whom correspondence should be addressed: Cell Biology Group,
The Heart Research Institute, 145 Missenden Rd., Camperdown, New South
Wales 2050, Australia. Tel.: 61-2-9550-3560; Fax: 61-2-9550-3302; E-mail: a.baoutina@hri.org.au.
Copyright © 2000 by The American Society for Biochemistry and Molecular Biology, Inc.
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