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苏拉明可抑制兔主动脉内膜损伤后体内的内膜增厚。

Suramin inhibits intimal thickening following intimal injury in the rabbit aorta in vivo.

作者信息

Asada Y, Tsuneyoshi A, Marutsuka K, Sumiyoshi A

机构信息

First Department of Pathology, Miyazaki Medical College, Japan.

出版信息

Cardiovasc Res. 1994 Aug;28(8):1166-9. doi: 10.1093/cvr/28.8.1166.

DOI:10.1093/cvr/28.8.1166
PMID:7954618
Abstract

OBJECTIVE

Proliferation of vascular smooth muscle cells is a major event in atherogenesis. Several growth factors have been well documented to control this proliferation. Inhibition by suramin of the binding of some growth factors to their receptors has recently been reported. The aim of this study was to examine the effects of this agent on neointimal thickening following intimal mechanical injury, as well as on platelet function.

METHODS

Intimal thickening was induced by indwelling of polyethylene tubing for 24 h in the rabbit aorta. Rabbits were killed 10 d after drawing out the tubing. Throughout the experiment, suramin (15 mg.kg-1) was injected intravenously every 24 h. Morphological and morphometrical studies were performed in the suramin treated group (n = 6) and in a control group (n = 6). Platelet-rich plasma was prepared from animals before and 3 h after injection of suramin. Platelet aggregation and ATP release induced by collagen were examined. Platelet adhesion on the de-endothelialised area of the rabbit aorta was also examined in the two groups.

RESULTS

The mean intimal thickening in the suramin treated group was significantly less than in the control group. Smooth muscle cell replication and cell density in the thickened intima of the suramin treated group were less than in control. Suramin did not affect collagen induced platelet aggregation, ATP release, or platelet adhesion.

CONCLUSIONS

Suramin has an inhibitory effect on the neointimal thickening and intimal smooth muscle cell proliferation after intimal injury in the rabbit aorta, but has no effect on platelet function.

摘要

目的

血管平滑肌细胞增殖是动脉粥样硬化形成过程中的一个主要事件。已有充分文献证明几种生长因子可控制这种增殖。最近有报道称,苏拉明可抑制某些生长因子与其受体的结合。本研究的目的是检验该药物对内膜机械损伤后新生内膜增厚以及血小板功能的影响。

方法

通过在兔主动脉内留置聚乙烯管24小时诱导内膜增厚。拔出管子10天后处死兔子。在整个实验过程中,每24小时静脉注射一次苏拉明(15毫克/千克)。对苏拉明治疗组(n = 6)和对照组(n = 6)进行形态学和形态计量学研究。从注射苏拉明前及注射后3小时的动物体内制备富含血小板的血浆。检测胶原诱导的血小板聚集和ATP释放情况。还在两组中检测了血小板在兔主动脉去内皮区域的黏附情况。

结果

苏拉明治疗组的平均内膜增厚明显小于对照组。苏拉明治疗组增厚内膜中的平滑肌细胞复制和细胞密度低于对照组。苏拉明不影响胶原诱导的血小板聚集、ATP释放或血小板黏附。

结论

苏拉明对兔主动脉内膜损伤后的新生内膜增厚和内膜平滑肌细胞增殖有抑制作用,但对血小板功能无影响。

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