首页> 美国卫生研究院文献>The Journal of Clinical Investigation >Platelet-derived growth factor activity and mRNA expression in healing vascular grafts in baboons. Association in vivo of platelet-derived growth factor mRNA and protein with cellular proliferation.
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Platelet-derived growth factor activity and mRNA expression in healing vascular grafts in baboons. Association in vivo of platelet-derived growth factor mRNA and protein with cellular proliferation.

机译:狒狒愈合血管移植物中的血小板衍生生长因子活性和mRNA表达。血小板衍生的生长因子mRNA和蛋白质在体内与细胞增殖的关联。

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摘要

In a baboon graft model of arterial intimal thickening, smooth muscle cells (SMC) have been observed to proliferate underneath an intact monolayer of endothelium and in the absence of platelet adherence. Because platelets are not present and therefore cannot be a major source of growth stimulus, we have proposed that the vascular wall cells in the graft intima express mitogens and regulate SMC proliferation. To test this hypothesis, we assayed the grafts for mitogenic activity and expression of growth factor genes. Segments of healing graft and of normal artery, when perfused ex vivo, released mitogenic activity into the perfusate. The graft released more mitogen than the normal arterial segment, and some of the activity was inhibitable with an antibody to human platelet-derived growth factor (PDGF). In addition, Northern analysis of total RNA demonstrated higher expression of PDGF-A chain mRNA in the graft intima compared to normal artery. PDGF-B chain mRNA was barely detectable in both tissues. PDGF mRNA levels within the graft interstices were not measured. In situ hybridization of 7.5- or 12-wk grafts indicated that some luminal endothelial cells and adjacent intimal SMC contained PDGF-A chain mRNA. By thymidine autoradiography, intimal SMC were observed to be proliferating in the inner third of the intima. These data demonstrate a difference in the pattern of PDGF transcript expression and luminal perfusate activity in graft as compared with control arteries. The association of intimal smooth muscle cell proliferation with intimal PDGF mRNA expression and release of PDGF-like protein supports the hypothesis that factors from cells that have grown into the graft or populated its surface rather than platelets may regulate intimal smooth muscle cell proliferation in this model.
机译:在狒狒的动脉内膜增厚移植模型中,已观察到平滑肌细胞(SMC)在完整的内皮单层下增殖并且没有血小板粘附。由于血小板不存在,因此不能成为生长刺激的主要来源,因此我们提出移植物内膜中的血管壁细胞表达促细胞分裂剂并调节SMC增殖。为了检验该假设,我们分析了移植物的促有丝分裂活性和生长因子基因的表达。当离体灌注时,愈合移植物和正常动脉的部分将有丝分裂活性释放到灌注液中。移植物释放的促分裂原比正常动脉节段更多,某些活性被人血小板源性生长因子(PDGF)抗体抑制。此外,总RNA的Northern分析表明,与正常动脉相比,PDGF-A链mRNA在移植内膜中的表达更高。在两个组织中都几乎检测不到PDGF-B链mRNA。没有测量移植物间隙中的PDGF mRNA水平。 7.5或12周移植物的原位杂交表明,一些腔内皮细胞和邻近的内膜SMC含有PDGF-A链mRNA。通过胸苷放射自显影术,观察到内膜SMC在内膜的内部三分之一中增殖。这些数据证明了与对照动脉相比,PDGF转录本表达模式和管腔灌注液活性的差异。内膜平滑肌细胞增殖与内膜PDGF mRNA表达和PDGF样蛋白的释放之间的联系支持以下假说:在此模型中,来自已植入移植物中或填充其表面而不是血小板的细胞中的因素可能会调节内膜平滑肌细胞增殖。 。

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