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首页> 外文期刊>Journal of vascular research >Vascular cell kinetics in response to intimal injury ex vivo.
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Vascular cell kinetics in response to intimal injury ex vivo.

机译:离体对内膜损伤的响应的血管细胞动力学。

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摘要

BACKGROUND: Recent studies indicate that the smooth muscle-like cells contributing to neointimal hyperplasia after vascular injury derive from circulating precursor cells. Here, we define the time course of precursor cell influx, the roles of separate vascular layers, and the relative role of migration versus proliferation to intimal hyperplasia. METHODS AND RESULTS: After rat aortic denudation injury the neointimal cell number increased several 100-fold between days 4 and 28, preceded by a 5-fold increase in the number of adventitial cells and a 4-fold increase in the number of adventitial microvessels. The influx, migration, and maturation of neointimal cells were quantitated by culturing whole vessel explants at different time points after injury. Explant outgrowth increased 14-fold, and cell migration 3.5-fold on days 2-14 after injury. Cell proliferation increased less than 2-fold. The frequency of precursors to outgrowing cells, determined using limiting dilution analysis, increased 8-fold between days 2 and 4 after injury. Many outgrowing cells displayed characteristics of undifferentiated cells. CONCLUSIONS: Adventitial activation precedes development of the neointima, and precursor cell influx occurs on days 2-14 after injury. Cell migration, more than proliferation, contributes to fibrointimal dysplasia. These findings underline the importance of early therapeutic intervention with antimigratory compounds to prevent neointimal hyperplasia.
机译:背景:最近的研究表明,血管损伤后导致新内膜增生的平滑肌样细胞源于循环的前体细胞。在这里,我们定义了前体细胞涌入的时间过程,单独的血管层的作用以及相对于内膜增生的迁移与增殖的相对作用。方法和结果:在大鼠主动脉剥脱损伤后,新内膜细胞数目在第4天和第28天之间增加了几百倍,其中外膜细胞的数目增加了5倍,外膜微血管的数目增加了4倍。通过损伤后不同时间培养全血管外植体来定量新内膜细胞的流入,迁移和成熟。受伤后第2-14天,外植体的生长增加了14倍,而细胞迁移则增加了3.5倍。细胞增殖增加不到2倍。通过有限稀释分析确定的前体细胞生长的频率在损伤后第2天和第4天之间增加了8倍。许多向外生长的细胞表现出未分化细胞的特征。结论:新生内膜形成之前先进行性激活,损伤后2-14天发生前体细胞大量涌入。细胞迁移,而不是增殖,是导致纤维内膜异常增生的原因。这些发现强调了早期使用抗迁移化合物进行治疗干预以预防新内膜增生的重要性。

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