ENHANCED LDL OXIDATION IN UREMIC PATIENTS - AN ADDITIONAL MECHANISM FOR ACCELERATED ATHEROSCLEROSIS

被引：252

作者：

MAGGI, E

BELLAZZI, R

FALASCHI, F

FRATTONI, A

PERANI, G

FINARDI, G

GAZO, A

NAI, M

ROMANINI, D

BELLOMO, G

机构：

[1] UNIV PAVIA, POLICLIN SAN MATTEO,IRCCS,MED CLIN 1, DEPT INTERNAL MED, I-27100 PAVIA, ITALY

[2] UNIV TORINO, DEPT EXPTL MED & ONCOL, TURIN, ITALY

[3] USSL 78, NEPHROL & DIALYSIS, VIGEVANO, ITALY

来源：

KIDNEY INTERNATIONAL | 1994年 / 45卷 / 03期

关键词：

D O I：

10.1038/ki.1994.115

中图分类号：

R5 [内科学]; R69 [泌尿科学（泌尿生殖系疾病）];

学科分类号：

1002 ; 100201 ;

摘要：

Since oxidized low-density lipoprotein (LDL) is more atherogenic than native LDL, LDL oxidation was investigated in uremic patients who often develop accelerated atherogenesis. Three groups of uremic patients were studied (10 on predialysis conservative therapy, 11 on repetitive hemodialysis, 13 on peritoneal dialysis) and compared with seventy matched controls. LDL oxidation was evaluated in all patients as: (i) the susceptibility to in vitro oxidation (by measuring the resistence to Cu++-induced formation of conjugated dienes), (ii) vitamin E concentration in LDL, and (iii) presence of plasma anti-oxidized LDL antibodies, expressed as the ratio antio-xLDL/anti-nativeLDL antibodies. The lipid profile was studied in all patients. Vitamin E concentration did not differ between the various groups, although LDL from uremic patients appeared more susceptible to in vitro and in vivo oxidation (as demonstrated by an earlier generation of conjugated dienes and by the presence of an higher antibody ratio) compared to control subjects. Subclass analysis of the different patients revealed that peritoneal dialysis treatment ameliorated the oxidation markers. However, a prolonged dialytic treatment caused a decrease in vitamin E concentration in LDL and increased their susceptibility to oxidation.

引用

页码：876 / 883

页数：8

共 34 条

[1] Alaupovic P, 1988, Adv Exp Med Biol, V243, P289
[2] REACTIVE OXYGEN MOLECULES, OXIDANT INJURY AND RENAL-DISEASE
ANDREOLI, SP
[J]. PEDIATRIC NEPHROLOGY, 1991, 5 (06) : 733 - 742
[3] ATTMAN PO, 1991, KIDNEY INT, V39, pS16
[4] PRESENCE OF A MODIFIED LOW-DENSITY LIPOPROTEIN IN HUMANS
AVOGARO, P
BON, GB
CAZZOLATO, G
[J]. ARTERIOSCLEROSIS, 1988, 8 (01): : 79 - 87
[5] MINIMALLY MODIFIED LOW-DENSITY-LIPOPROTEIN STIMULATES MONOCYTE ENDOTHELIAL INTERACTIONS
BERLINER, JA
TERRITO, MC
SEVANIAN, A
RAMIN, S
KIM, JA
BAMSHAD, B
ESTERSON, M
FOGELMAN, AM
[J]. JOURNAL OF CLINICAL INVESTIGATION, 1990, 85 (04) : 1260 - 1266
[6] EFFECT OF DIETARY MONOUNSATURATED AND POLYUNSATURATED FATTY-ACIDS ON THE SUSCEPTIBILITY OF PLASMA LOW-DENSITY LIPOPROTEINS TO OXIDATIVE MODIFICATION
BONANOME, A
PAGNAN, A
BIFFANTI, S
OPPORTUNO, A
SORGATO, F
DORELLA, M
MAIORINO, M
URSINI, F
[J]. ARTERIOSCLEROSIS AND THROMBOSIS, 1992, 12 (04): : 529 - 533
[7] BOYD HC, 1989, AM J PATHOL, V135, P815
[8] PREVALENCE OF SERUM-LIPID ABNORMALITIES IN CHRONIC-HEMODIALYSIS
BRUNZELL, JD
ALBERS, JJ
HAAS, LB
GOLDBERG, AP
AGADOA, L
SHERRARD, DJ
[J]. METABOLISM-CLINICAL AND EXPERIMENTAL, 1977, 26 (08): : 903 - 910
[9] ANTIATHEROGENIC EFFECT OF PROBUCOL UNRELATED TO ITS HYPOCHOLESTEROLEMIC EFFECT - EVIDENCE THAT ANTIOXIDANTS INVIVO CAN SELECTIVELY INHIBIT LOW-DENSITY-LIPOPROTEIN DEGRADATION IN MACROPHAGE-RICH FATTY STREAKS AND SLOW THE PROGRESSION OF ATHEROSCLEROSIS IN THE WATANABE HERITABLE HYPERLIPIDEMIC RABBIT
CAREW, TE
SCHWENKE, DC
STEINBERG, D
[J]. PROCEEDINGS OF THE NATIONAL ACADEMY OF SCIENCES OF THE UNITED STATES OF AMERICA, 1987, 84 (21) : 7725 - 7729
[10] COOKSON FB, 1971, BRIT J EXP PATHOL, V52, P62

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