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首页> 外文期刊>Blood: The Journal of the American Society of Hematology >Acute and severe coagulopathy in adult mice following silencing of hepatic antithrombin and protein C production.
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Acute and severe coagulopathy in adult mice following silencing of hepatic antithrombin and protein C production.

机译:肝抗凝血酶和蛋白C产生沉默后,成年小鼠急性和严重凝血病。

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摘要

Mice deficient in the anticoagulants antithrombin (Serpinc1) or protein C (Proc) display premature death due to thrombosis-related coagulopathy, thereby precluding their use in gene function studies and thrombosis models. We used RNA interference to silence Serpinc1 and/or Proc in normal adult mice. The severe coagulopathy that followed combined "knockdown" of these genes is reported. Two days after siRNA injection, thrombi (occlusive) were observed in vessels (large and medium-sized) in multiple tissues, and hemorrhages were prominent in the ocular, mandibular, and maxillary areas. Tissue fibrin deposition and reduction of plasma fibrinogen accompanied this phenotype. The coagulopathy was prevented by dabigatran etexilate treatment. Silencing of Serpinc1 alone yielded a comparable but milder phenotype with later onset. The phenotype was absent when Proc was targeted alone. We conclude that RNA interference of Serpinc1 and/or Proc allows for evaluation of the function of these genes in vivo and provides a novel, controlled mouse model for spontaneous venous thrombosis.
机译:缺乏抗凝血酶抗凝血酶(Serpinc1)或蛋白C(Proc)的小鼠由于与血栓形成有关的凝血病而显示过早死亡,从而排除了它们在基因功能研究和血栓形成模型中的用途。我们使用RNA干扰沉默正常成年小鼠的Serpinc1和/或Proc。据报道,这些基因联合“击倒”后出现严重的凝血病。 siRNA注射后两天,在多个组织的血管(大中型)中观察到血栓(闭塞),并且眼,下颌和上颌区的出血明显。组织纤维蛋白沉积和血浆纤维蛋白原的减少伴随着该表型。达比加群酯治疗可预防凝血病。单独沉默Serpinc1产生了可比但较轻的表型,但起病较晚。当单独针对Proc时,不存在该表型。我们得出结论,Serpinc1和/或Proc的RNA干扰允许评估这些基因在体内的功能,并为自发性静脉血栓形成提供一种新型的受控小鼠模型。

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