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凝血因子XI在人深静脉血栓中的定位以及活化凝血因子XI对静脉血栓形成和止血的作用。

Factor XI localization in human deep venous thrombus and function of activated factor XI on venous thrombus formation and hemostasis.

作者信息

Oguri Nobuyuki, Gi Toshihiro, Nakamura Eriko, Maekawa Kazunari, Furukoji Eiji, Okawa Hoshimi, Kouyama Sho, Horiuchi Saki, Sawaguchi Akira, Sakae Tatefumi, Azuma Minako, Asada Yujiro, Yamashita Atsushi

机构信息

Department of Pathology, Faculty of Medicine, University of Miyazaki, Miyazaki, Japan.

Department of Radiology, Faculty of Medicine, University of Miyazaki, Miyazaki, Japan.

出版信息

Res Pract Thromb Haemost. 2025 Mar 3;9(2):102720. doi: 10.1016/j.rpth.2025.102720. eCollection 2025 Feb.

Abstract

BACKGROUND

Novel anticoagulants targeting coagulation factor (F)XI/activated FXI (FXIa) are currently under development. However, whether FXI is present in human deep vein thrombosis (DVT) and whether FXIa and activated FX (FXa) play different roles in venous thrombus formation and hemostasis remain unclear.

OBJECTIVES

To determine the presence of FXI in DVT and the effects of direct oral FXIa and FXa inhibitors on venous thrombus formation and hemostasis in rabbits and on thrombus formation.

METHODS

We immunohistochemically assessed FXI localization in human-aspirated DVT ( = 15). Additionally, we compared thrombus formation induced by endothelial denudation and stenosis or stasis in the jugular vein and skin bleeding time and volume between rabbits treated with direct FXIa inhibitors (ONO-1600586) and FXa inhibitors (rivaroxaban). rabbit and human blood were perfused in a flow chamber under low-shear rates (70/s).

RESULTS

FXI was localized in all DVT, predominantly in fibrin-rich areas. The FXI immunopositive area in the nonorganizing area was greater than that in the organizing area. Although FXIa and FXa inhibitors comparably inhibited venous thrombus formation, FXIa inhibitors did not affect bleeding time or volume in rabbits. FXIa or FXa inhibitors mildly or strongly inhibited fibrin formation at low-shear rates, respectively. Furthermore, the FXIa inhibitor suppressed human FXIa activity, thrombin generation, and fibrin formation during perfusion.

CONCLUSION

The pathologic findings of human DVT suggest FXI's role in human DVT. FXIa inhibitors may inhibit less fibrin formation than FXa inhibitors and may explain the minor role of FXIa in hemostasis.

摘要

背景

目前正在研发针对凝血因子(F)XI/活化FXI(FXIa)的新型抗凝剂。然而,FXI是否存在于人类深静脉血栓形成(DVT)中,以及FXIa和活化FX(FXa)在静脉血栓形成和止血过程中是否发挥不同作用仍不清楚。

目的

确定FXI在DVT中的存在情况,以及直接口服FXIa和FXa抑制剂对家兔静脉血栓形成和止血以及血栓形成的影响。

方法

我们采用免疫组织化学方法评估FXI在人抽吸DVT(n = 15)中的定位。此外,我们比较了直接FXIa抑制剂(ONO-1600586)和FXa抑制剂(利伐沙班)处理的家兔颈静脉内皮剥脱和狭窄或淤滞诱导的血栓形成以及皮肤出血时间和出血量。在家兔和人血液在低剪切速率(70/s)下在流动腔中灌注。

结果

FXI定位于所有DVT中,主要位于富含纤维蛋白的区域。非机化区域的FXI免疫阳性面积大于机化区域。虽然FXIa和FXa抑制剂对静脉血栓形成的抑制作用相当,但FXIa抑制剂对家兔的出血时间或出血量没有影响。FXIa或FXa抑制剂分别在低剪切速率下轻度或强烈抑制纤维蛋白形成。此外,FXIa抑制剂在灌注过程中抑制人FXIa活性、凝血酶生成和纤维蛋白形成。

结论

人类DVT的病理结果提示FXI在人类DVT中的作用。FXIa抑制剂可能比FXa抑制剂抑制更少的纤维蛋白形成,这可能解释了FXIa在止血中的次要作用。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/8c1d/11999338/99bde8739439/ga1.jpg

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