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重组因子VIIa变体(NN1731)对健康志愿者和血友病患者全血中血小板功能、血凝块结构及力起始时间的影响。

Effect of recombinant factor VIIa variant (NN1731) on platelet function, clot structure and force onset time in whole blood from healthy volunteers and haemophilia patients.

作者信息

Brophy D F, Martin E J, Nolte M E, Kuhn J G, Carr M E

机构信息

Coagulation Special Studies Laboratory, Department of Pharmacy of Virginia Commonwealth University, Richmond, VA 23298, USA.

出版信息

Haemophilia. 2007 Sep;13(5):533-41. doi: 10.1111/j.1365-2516.2007.01524.x.

Abstract

NN1731 is a novel variant of recombinant factor VIIa (rFVIIa) that binds to activated platelets, but has greater enzymatic activity than rFVIIa in generating FXa and thrombin. The effect of NN1731 on clot structure and platelet function was characterized ex vivo in whole blood from healthy volunteers and haemophilic patients. Blood samples from six healthy volunteers, nine haemophilia A patients with and without inhibitors and one acquired haemophilia A patient, were spiked with increasing concentrations (0.32, 0.64 and 1.28 microg mL(-1)) of rFVIIa and NN1731. Platelet contractile force (PCF) or platelet function, clot elastic modulus (CEM) or clot structure, and force onset time (FOT) or the thrombin generation time (TGT) were determined using the Hemodyne Hemostasis Analysis System (HAS). Baseline PCF, CEM and FOT values in patients were abnormal compared to healthy volunteers' baseline values. Overall, haemophilia blood samples with or without inhibitors spiked with NN1731 had significantly greater PCF, CEM and shorter FOT values relative to samples spiked with corresponding doses of rFVIIa. The variability in response to treatment between patients was greater with rFVIIa compared to NN1731. At 1.28 microg mL(-1) (90 microg kg(-1)), NN1731 normalized PCF, CEM and FOT in nine of 10 patients, while rFVIIa normalized these parameters in four of 10 patients. Increasing in vitro concentrations of NN1731 normalized platelet function, clot structure and thrombin generation consistently in haemophilia blood with or without inhibitors. NN1731 may be a promising haemostatic agent for patients with bleeding disorders. These results should be confirmed in an in vivo study.

摘要

NN1731是重组因子VIIa(rFVIIa)的一种新型变体,它能与活化血小板结合,但在生成FXa和凝血酶方面比rFVIIa具有更高的酶活性。在健康志愿者和血友病患者的全血中对NN1731对凝块结构和血小板功能的影响进行了体外研究。采集了6名健康志愿者、9名有或无抑制剂的甲型血友病患者以及1名获得性甲型血友病患者的血样,分别加入浓度递增(0.32、0.64和1.28μg mL⁻¹)的rFVIIa和NN1731。使用Hemodyne止血分析系统(HAS)测定血小板收缩力(PCF)或血小板功能、凝块弹性模量(CEM)或凝块结构以及力起始时间(FOT)或凝血酶生成时间(TGT)。与健康志愿者的基线值相比,患者的基线PCF、CEM和FOT值异常。总体而言,与加入相应剂量rFVIIa的样本相比,加入NN1731的有或无抑制剂的血友病血样具有显著更高的PCF、CEM值和更短的FOT值。与NN1731相比,rFVIIa治疗后患者之间的反应变异性更大。在1.28μg mL⁻¹(90μg kg⁻¹)时,NN1731使10名患者中的9名患者的PCF、CEM和FOT恢复正常,而rFVIIa使10名患者中的4名患者的这些参数恢复正常。在有或无抑制剂的血友病血液中,体外增加NN1731的浓度可使血小板功能、凝块结构和凝血酶生成持续恢复正常。NN1731可能是一种有前途的用于出血性疾病患者的止血剂。这些结果应在体内研究中得到证实。

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