LOW- AND HIGH-DENSITY-LIPOPROTEINS AS MITOGENIC FACTORS FOR VASCULAR SMOOTH-MUSCLE CELLS - INDIVIDUAL, ADDITIVE AND SYNERGISTIC EFFECTS

被引:19
作者
RESINK, TJ [1 ]
BOCHKOV, VN [1 ]
HAHN, AWA [1 ]
PHILIPPOVA, MP [1 ]
BUHLER, FR [1 ]
TKACHUK, VA [1 ]
机构
[1] CARDIOVASC RES CTR,INST EXPTL CARDIOL,MOLEC ENDOCRINOL LAB,MOSCOW,RUSSIA
来源
JOURNAL OF VASCULAR RESEARCH | 1995年 / 32卷 / 05期
关键词
DNA SYNTHESIS; LIPOPROTEINS; NATIVE; PROTEIN SYNTHESIS; VASCULAR SMOOTH MUSCLE CELL; PROLIFERATION; GROWTH FACTORS;
D O I
10.1159/000159107
中图分类号
Q4 [生理学];
学科分类号
071003 ;
摘要
The mitogenic activities of low (LDL)- and high (HDL)-density lipoproteins have been examined in cultures of human vascular smooth muscle cells (VSMC). LDL and HDL(3) dose-dependently (EC(50) values similar to 50 mu g/ml) stimulated DNA and protein synthesis ([H-3]-thymidine and [H-3]-leucine incorporation, respectively) in the absence of exogenously added mitogens. The synthetic responses of VSMC to combinations of LDL and HDL(3) were additive, indicating that each lipoprotein mediates discrete effects. LDL or HDL(3) promoted VSMC proliferation under strict mitogen-free conditions, but this growth response was not sustained. VSMC exposed to combinations of lipoproteins (either LDL or HDL(3)) and growth factors (either PDGF-BB, EGF, bFGF or IGF) exhibited synergistic DNA synthesis responses. In the combined presence of PDGF-BB and either LDL or HDL(3), VSMC proliferation was sustained. Anionized lipoprotein preparations (oxidized, acetylated, carbamylated or malonimylated) also stimulated DNA and protein synthesis. Since the antioxidant beta-hydroxylated toluene did not block the effect of native LDL on DNA synthesis, and fucoidin, a specific competitor for the 'scavenger' receptor, did not inhibit. oxidized LDL-induced DNA synthesis, activation of mitogenic signals by lipoproteins does not depend on lipid peroxidation. Rather, the apparent intrinsic mitogenic potential of lipoproteins may depend upon their direct activation of replication-coupled signal transduction systems.
引用
收藏
页码:328 / 338
页数:11
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