Fager G, Camejo G, Bondjers G
Wallenberg Laboratory for Cardiovascular Research, Faculty of Medicine, University of Göteborg, Sweden.
In Vitro Cell Dev Biol. 1992 Mar;28A(3 Pt 1):168-75. doi: 10.1007/BF02631087.
We have investigated the effects of interactions between growth factors and heparin-like glycosaminoglycans on untransformed human arterial smooth muscle cells (hASMC) in vitro. The results indicate that heparin in the presence of serum mitogens prevents the cells from entering the S phase of the cell cycle by binding and inactivating reversibly some serum mitogen(s). Our results suggest that platelet-derived growth factor (PDGF) is one of them and that it is the most potent stimulator of hASMC growth in vitro. Thymidine incorporation as well as increase in DNA content was inhibited not only by the presence of heparin in serum-containing medium but also when serum was chromatographed on Heparin-Sepharose at physiologic salt concentrations before exposure to the cells. The mitogenic activity of the unretained serum fraction was restored by the addition of PDGF AA, AB, or BB dimers or of a fraction (RF I) that dissociated from Heparin-Sepharose at 0.2 to 0.6 M NaCl. Radiolabeled recombinant PDGF (c-sis) dissociated from Heparin-Sepharose within a concentration range of NaCl similar to that of RF I. Neither the unretained material nor the RF I or PDGF dimers were effective alone. The effect of RF I was significantly decreased by the addition of an anti-PDGF IgG that is known to neutralize the PDGF mitogenic activity partially. Addition of heparin abolished DNA-synthesis when the PDGF dimers or RF I were combined with the unretained fraction. A second fraction (RF II) bound strongly to Heparin-Sepharose and eluted between 1.1 and 1.6 M NaCl. The RF II also induced DNA synthesis but was neither as efficient as RF I nor depending on other serum fractions for growth promotion and it was not inhibited by anti-PDGF IgG. A similar strong affinity for Heparin-Sepharose was found for labeled basic fibroblast growth factor and we cannot exclude the possibility that RF II represent fibroblast growth factor. Under these culture conditions, inhibition of hASMC proliferation was directly correlated with the expression of smooth muscle specific alpha actin isoforms in stress fibers and the suppression of a proliferating cell-specific nuclear antigen. Conversely, stimulation of hASMC proliferation was associated with the opposite phenomenon. We conclude that heparin-like glycosaminoglycans influence growth and phenotype of hASMCs in vitro by binding and inactivating PDGF. Inasmuch as heparin-like substances constitute a significant proportion of the proteoglycan-associated glycosaminoglycans of the arterial wall, such mechanisms might be important for the development of atherosclerotic lesions.
我们已经在体外研究了生长因子与类肝素糖胺聚糖之间的相互作用对未转化的人动脉平滑肌细胞(hASMC)的影响。结果表明,在血清促细胞分裂剂存在的情况下,肝素通过结合并可逆地使某些血清促细胞分裂剂失活,从而阻止细胞进入细胞周期的S期。我们的结果表明,血小板衍生生长因子(PDGF)是其中之一,并且它是体外hASMC生长的最有效刺激物。不仅含血清培养基中存在肝素会抑制胸苷掺入以及DNA含量增加,而且在生理盐浓度下将血清在肝素-琼脂糖凝胶上进行层析后再暴露于细胞时也会出现这种情况。通过添加PDGF AA、AB或BB二聚体或在0.2至0.6 M NaCl浓度下从肝素-琼脂糖凝胶上解离的一个组分(RF I),未保留的血清组分的促有丝分裂活性得以恢复。放射性标记的重组PDGF(c-sis)在与RF I相似的NaCl浓度范围内从肝素-琼脂糖凝胶上解离。未保留的物质、RF I或PDGF二聚体单独使用均无效。添加已知可部分中和PDGF促有丝分裂活性的抗PDGF IgG后,RF I的作用显著降低。当PDGF二聚体或RF I与未保留的组分结合时,添加肝素会消除DNA合成。第二个组分(RF II)与肝素-琼脂糖凝胶紧密结合,并在1.1至1.6 M NaCl之间洗脱。RF II也可诱导DNA合成,但不如RF I有效,也不依赖于其他血清组分来促进生长,并且不受抗PDGF IgG的抑制。对于标记的碱性成纤维细胞生长因子,发现其对肝素-琼脂糖凝胶具有类似的强亲和力,我们不能排除RF II代表成纤维细胞生长因子的可能性。在这些培养条件下,hASMC增殖的抑制与应力纤维中平滑肌特异性α肌动蛋白同工型的表达以及增殖细胞特异性核抗原的抑制直接相关。相反,hASMC增殖的刺激与相反的现象相关。我们得出结论,类肝素糖胺聚糖通过结合并使PDGF失活来影响体外hASMC的生长和表型。由于类肝素物质在动脉壁的蛋白聚糖相关糖胺聚糖中占很大比例,这种机制可能对动脉粥样硬化病变的发展很重要。
