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首页> 外文期刊>Thrombosis Research: An International Journal on Vascular Obstruction, Hemorrhage and Hemostasis >The effect of anticoagulation with subcutaneously delivered polyethylene glycol conjugated hirudin and recombinant tissue plasminogen activator on recurrent stenosis in the rabbit double-balloon injury model.
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The effect of anticoagulation with subcutaneously delivered polyethylene glycol conjugated hirudin and recombinant tissue plasminogen activator on recurrent stenosis in the rabbit double-balloon injury model.

机译:皮下递送的聚乙二醇水hi素和重组组织纤溶酶原激活剂抗凝作用对兔双气囊损伤模型中反复狭窄的作用。

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摘要

Myointimal hyperplasia is the condition usually responsible for recurrent stenosis (restenosis) after endarterectomy, bypass grafting and angioplasty. Its cause is still not known. The present study examined whether inhibition of thrombin by tissue plasminogen activator (r-TPA) or polyethylene glycol recombinant hirudin (PEG-hirudin) could reduce restenosis in an animal model. Restenosis was induced in 20 cholesterol-fed rabbits. The right carotid artery underwent a double-balloon injury while left carotid artery acted as a control. Recombinant tissue plasminogen activator (1 mg kg(-1) s.c.) and PEG-hirudin (0.7 mg kg(-1) s.c.) were given subcutaneously with normal saline acting as a control. Blood levels of PEG-hirudin were measured by both ELISA and an Ecarin (activity) assay. Vessel dimensions were measured in histological sections, obtained from perfusion-fixed tissue, using computerised planimetry. The model reproduced many of the histological changes found in human restenosis, such as intramural thrombus, rupture of the elastic lamina, macrophage infiltration and smooth muscle migration. Reinjury caused an almost three-fold reduction in the area of the lumen (median 0.25 mm(2)) compared with uninjured vessels (median 0.72 mm(2)). The mean plasma levels of PEG-hirudin and r-tPA achieved were 291 ng/ml (S.E.M. 28 ng/ml) and 34 IU/ml (S.E.M. 12 IU/ml), respectively. PEG-hirudin significantly inhibited the effect of balloon injury on luminal area compared with saline-treated controls (0.21 versus 0.44 mm(2), respectively, P<0.05). Recombinant tPA also had a similar inhibitory affect, but this did not reach statistical significance (0.16 versus 0.44 mm(2), respectively, P>0.05). The magnitude of luminal narrowing was significantly reduced by subcutaneous injection of PEG-hirudin. Further studies are required to determine whether this effect can be enhanced by other antithrombins or improved methods of delivery.
机译:肌内膜增生通常是动脉内膜切除术,搭桥术和血管成形术后复发性狭窄(再狭窄)的病因。其原因仍然未知。本研究检查了通过组织纤溶酶原激活物(r-TPA)或聚乙二醇重组水rud素(PEG-hirudin)抑制凝血酶是否可以减少动物模型中的再狭窄。在20只胆固醇喂养的兔子中诱发了再狭窄。右颈动脉受到双气囊损伤,而左颈动脉作为对照。皮下注射重组组织纤维蛋白溶酶原激活剂(1 mg kg(-1)s.c.)和PEG-水ud素(0.7 mg kg(-1)s.c.),皮下注射生理盐水作为对照。 PEG-hirudin的血液水平通过ELISA和Ecarin(活性)测定法进行测量。使用计算机化的平面测量法,从灌注固定的组织获得的组织学切片中测量血管尺寸。该模型再现了人类再狭窄中发现的许多组织学变化,例如壁内血栓,弹性椎板破裂,巨噬细胞浸润和平滑肌迁移。与未受伤的血管(中位数0.72 mm(2))相比,再损伤引起的管腔面积减少了将近三倍(中位数0.25 mm(2))。达到的PEG-hirudin和r-tPA的平均血浆水平分别为291 ng / ml(S.E.M. 28 ng / ml)和34 IU / ml(S.E.M. 12 IU / ml)。与生理盐水处理的对照组相比,PEG-hirudin显着抑制了球囊损伤对管腔面积的影响(分别为0.21和0.44 mm(2),P <0.05)。重组tPA也具有类似的抑制作用,但是没有达到统计学显着性(分别为0.16对0.44 mm(2),P> 0.05)。皮下注射PEG-水ud素可显着降低管腔变窄的幅度。需要进一步的研究以确定这种作用是否可以通过其他抗凝血酶或改善的递送方法来增强。

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