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使用阿梅氏缩窄环通过下腔静脉低灌注建立的深静脉血栓形成小鼠模型。

A mouse model of deep vein thrombosis by inferior vena cava hypoperfusion using ameroid constrictors.

作者信息

Tadokoro Hiroko, Ota Yukihide, Uomoto Mari, Koizume Shiro, Sato Shinya, Nakamura Yoshiyasu, Yoshihara Mitsuyo, Endo-Takahashi Yoko, Negishi Yoichi, Miyagi Etsuko, Miyagi Yohei

机构信息

Molecular Pathology and Genetics Division, Kanagawa Cancer Center Research Institute, 2-3-2 Nakao, Asahi-ku, Yokohama, 241-8515, Kanagawa, Japan.

Department of Pathology, Kanagawa Cancer Center Hospital, 2-3-2 Nakao, Asahi-ku, Yokohama, 241- 8515, Kanagawa, Japan.

出版信息

Sci Rep. 2025 Jan 6;15(1):928. doi: 10.1038/s41598-024-84443-8.

Abstract

Traditional mouse models for deep vein thrombosis (DVT), frequently utilized in research focused on cancer-associated thrombosis (CAT), reliably induce thrombus formation by obstructing blood flow (BF) in the inferior vena cava (IVC), which does not occur in humans. Therefore, to develop a new DVT model for CAT studies, we implanted an ameroid constrictor (AC), a hygroscopic casein C-shape device, around the IVC and aorta of immunocompromised mice. We evaluated the thrombus 3 and 8 days post-AC implantation and compared it with the traditional model 2 days post-vena cava ligation. The size of each thrombus was measured, and the composition was assessed using histological staining; BF through the IVC was confirmed using ultrasound imaging. The thrombus size variability in the AC and ligation models was equivalent. Compared with thrombi on day 3 post-AC implantation, those on day 8 showed characteristics of human thrombi in the subacute to chronic stage. The BF in the IVC was maintained even on day 8. In summary, the AC model showed reproducibility with no significant difference in thrombus size variability from the traditional ligation model while maintaining the BF of the IVC.

摘要

传统的深静脉血栓形成(DVT)小鼠模型常用于专注于癌症相关血栓形成(CAT)的研究,通过阻塞下腔静脉(IVC)中的血流(BF)可靠地诱导血栓形成,而这在人类中不会发生。因此,为了开发一种用于CAT研究的新DVT模型,我们在免疫受损小鼠的IVC和主动脉周围植入了一种类淀粉样缩窄器(AC),一种吸湿性酪蛋白C形装置。我们在AC植入后3天和8天评估血栓,并将其与腔静脉结扎后2天的传统模型进行比较。测量每个血栓的大小,并使用组织学染色评估其组成;通过超声成像确认通过IVC的BF。AC模型和结扎模型中的血栓大小变异性相当。与AC植入后第3天的血栓相比,第8天的血栓表现出亚急性至慢性期人类血栓的特征。即使在第8天,IVC中的BF也得以维持。总之,AC模型显示出可重复性,与传统结扎模型相比,血栓大小变异性无显著差异,同时维持了IVC的BF。

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