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首页> 外文期刊>Thrombosis and Haemostasis: Journal of the International Society on Thrombosis and Haemostasis >Functional analyses of patient-derived IgG monoclonal anticardiolipin antibodies using in vivo thrombosis and in vivo microcirculation models.
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Functional analyses of patient-derived IgG monoclonal anticardiolipin antibodies using in vivo thrombosis and in vivo microcirculation models.

机译:使用体内血栓形成和体内微循环模型对患者来源的IgG单克隆抗心磷脂抗体进行功能分析。

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摘要

Antiphospholipid antibodies (aPL) have been associated with thrombosis and pregnancy losses in patients diagnosed with antiphospholipid syndrome (APS) and enhance thrombus formation in vivo in mice, but the mechanism of thrombosis by aPL is not completely understood. It has been proposed that aPL may affect endothelial cell (EC) function and/or induce their activation, transforming their anticoagulant surface into procoagulant, thus predisposing to thrombosis. It has been proposed that aPL may affect EC cell function and/or induce their activation, transforming their anticoagulant surface into procoagulant, thus predisposing to thrombosis. This study proposes to test the hypotheses that some IgG anticardiolipins (IgG aCL) with thrombogenic properties in mice, exert their effects through activation of endothelium. We studied seven patient-derived monoclonal aCL for their thrombogenic properties in an in vivo pinch-induced thrombosis model, and their functional activities in activating EC by analyzing in vivo leukocyte adhesion to endothelium in microcirculation in venules in exposed murine cremaster muscle and in vitro adhesion molecule expression in cultured EC. The binding of the monoclonal aCL to EC was also tested. In addition to the previous identified thrombogenic IS2, four of the five new more IgG monoclonal aCL (from two patients) were found to be thrombogenic. Of these five thrombogenic aCL, three caused more in vivo leukocyte adhesion to EC in microcirculation, as compared to that induced by the H2 control human monoclonal IgG, and enhanced expression of adhesion molecules (particularly VCAM-1) on cultured EC. These data show that about 2/3 patient-derived IgG monoclonal aCL are thrombogenic and suggest that some thrombogenic IgG aCL exert their effects through activating EC.
机译:在诊断为抗磷脂综合症(APS)的患者中,抗磷脂抗体(aPL)与血栓形成和妊娠流失相关,并增强了小鼠体内的血栓形成,但尚未完全了解aPL的血栓形成机理。已经提出,aPL可影响内皮细胞(EC)的功能和/或诱导其活化,将其抗凝表面转化为促凝剂,从而易于形成血栓。已经提出,aPL可影响EC细胞功能和/或诱导其活化,将其抗凝表面转化为促凝剂,从而易于血栓形成。这项研究建议检验以下假设:一些具有血栓形成特性的IgG抗心磷脂(IgG aCL)通过激活内皮发挥其作用。我们通过分析体内白鼠对睾丸肌肉小静脉内微循环中白细胞对内皮的黏附作用以及体外黏附作用,研究了七种源自患者的单克隆aCL在体内捏诱导血栓形成模型中的血栓形成特性,以及它们在激活EC中的功能活性。分子在培养EC中的表达。还测试了单克隆aCL与EC的结合。除了先前确定的血栓形成性IS2之外,五个新的IgG单克隆aCL(来自两名患者)中的四个也被发现具有血栓形成性。在这五个血栓形成性aCL中,与H2对照人单克隆IgG诱导的相比,三个血栓形成性aCL在微循环中引起更多的体内白​​细胞对EC的粘附,并且在培养的EC上粘附分子(尤其是VCAM-1)的表达增强。这些数据表明约有2/3患者来源的IgG单克隆aCL具有血栓形成作用,并表明某些血栓形成的IgG aCL通过激活EC发挥作用。

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