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局部应用肝素对大鼠肠系膜微静脉内白细胞滚动及趋化因子诱导的牢固黏附的抑制作用

Inhibitory effect of locally administered heparin on leukocyte rolling and chemoattractant-induced firm adhesion in rat mesenteric venules in vivo.

作者信息

Xie X, Thorlacius H, Raud J, Hedqvist P, Lindbom L

机构信息

Department of Physiology and Pharmacology, Karolinska Institutet, Stockholm, Sweden.

出版信息

Br J Pharmacol. 1997 Nov;122(5):906-10. doi: 10.1038/sj.bjp.0701454.

Abstract
  1. Anti-inflammatory actions of heparin and related glycosaminoglycans have been described in the literature. Here, we used intravital microscopy of the rat mesentery microcirculation to examine effects of locally administered heparin on leukocyte rolling and chemoattractant-induced firm adhesion. 2. It was found that topical application of heparin reduced N-formyl-methionyl-leucyl-phenylalanine (fMLP)-induced leukocyte adhesion. Notably, the inhibitory action of heparin was not dose-dependent, but rather a biphasic dose-response was found, i.e. low (2 and 20 iu ml(-1)) and high (1000 iu ml(-1)) concentrations of heparin significantly reduced adhesion, whereas an intermediate dose (200 iu ml(-1)) was less effective. 3. Heparin, 2 and 20 iu ml(-1), decreased rolling leukocyte flux, while having no effect on blood flow or total leukocyte flux. By contrast, heparin, 200 and 1000 iu ml(-1), increased total leukocyte flux in parallel with a rise in volume blood flow resulting in recovery of the rolling leukocyte flux at these doses. Thus, the biphasic inhibitory action of heparin on fMLP-induced firm adhesion could in part be attributed to changes in leukocyte delivery (i.e. blood flow) and rolling leukocyte flux induced by heparin. 4. When compensating for the influence of different rolling levels on fMLP-evoked adhesion, a dose-related inhibitory effect of heparin on the firm adhesive response per se was revealed. Similar results were obtained in a static adhesion assay in vitro where heparin 200 and 1000 iu ml(-1) (but not 2 and 20 iu ml(-1)) significantly inhibited fMLP-induced leukocyte adhesion in the absence of any modulatory influence on changes in rolling. 5. Our data show that locally administered heparin inhibits leukocyte rolling as well as chemoattractant-induced firm adhesion in vivo which thus may contribute to the postulated anti-inflammatory activity of this compound. However, because of interference with several microvascular functions, strict dose-dependent responses to heparin treatment were not found, which illustrates the complex interplay between local blood flow, leukocyte rolling and chemoattractant-induced adhesion as determinants of leukocyte recruitment to tissues in inflammation.
摘要
  1. 肝素及相关糖胺聚糖的抗炎作用已在文献中有所描述。在此,我们利用大鼠肠系膜微循环的活体显微镜检查来研究局部应用肝素对白细胞滚动以及趋化因子诱导的牢固黏附的影响。2. 研究发现,局部应用肝素可降低N-甲酰甲硫氨酰-亮氨酰-苯丙氨酸(fMLP)诱导的白细胞黏附。值得注意的是,肝素的抑制作用并非剂量依赖性,而是呈现双相剂量反应,即低浓度(2和20国际单位/毫升)和高浓度(1000国际单位/毫升)的肝素可显著降低黏附,而中等剂量(200国际单位/毫升)的效果较差。3. 2和20国际单位/毫升的肝素可降低滚动白细胞通量,而对血流或总白细胞通量无影响。相比之下,200和1000国际单位/毫升的肝素可使总白细胞通量增加,同时伴随血容量增加,从而使这些剂量下的滚动白细胞通量恢复。因此,肝素对fMLP诱导的牢固黏附的双相抑制作用部分可归因于肝素诱导的白细胞输送(即血流)和滚动白细胞通量的变化。4. 当补偿不同滚动水平对fMLP诱发黏附的影响时,发现肝素对牢固黏附反应本身具有剂量相关的抑制作用。在体外静态黏附试验中也获得了类似结果,在该试验中,200和1000国际单位/毫升(而非2和20国际单位/毫升)的肝素在对滚动变化无任何调节影响的情况下,显著抑制了fMLP诱导的白细胞黏附。5. 我们的数据表明,局部应用肝素可在体内抑制白细胞滚动以及趋化因子诱导的牢固黏附,这可能有助于该化合物假定的抗炎活性。然而,由于对多种微血管功能的干扰,未发现对肝素治疗的严格剂量依赖性反应,这说明了局部血流、白细胞滚动和趋化因子诱导的黏附之间复杂的相互作用,这些因素是炎症中白细胞募集到组织的决定因素。

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