血管性血友病因子和P-选择素在内毒素血症微血管血栓形成中的不同作用

Differential role of von Willebrand factor and P-selectin on microvascular thrombosis in endotoxemia.

作者信息

Patel Kavita N, Soubra Said H, Bellera Ricardo V, Dong Jing-Fei, McMullen Colleen A, Burns Alan R, Rumbaut Rolando E

机构信息

Department of Pediatrics, Baylor College of Medicine, Houston, TX 77030.

Medical Care Line, Michael E. DeBakey VA Medical Center, Houston, TX 77030.

出版信息

Arterioscler Thromb Vasc Biol. 2008 Dec;28(12):2225-2230. doi: 10.1161/ATVBAHA.108.175679. Epub 2008 Sep 18.

DOI:10.1161/ATVBAHA.108.175679

PMID:18802014

原文链接:https://pmc.ncbi.nlm.nih.gov/articles/PMC2585611/

Abstract

OBJECTIVE

Endotoxin (lipopolysaccharide [LPS]) enhances microvascular thrombosis in mouse cremaster venules. Because von Willebrand factor (vWF) and P-selectin are suggested to mediate LPS-induced platelet-microvessel interactions, we determined whether vWF and P-selectin contribute to microvascular thrombosis in endotoxemia.

METHODS AND RESULTS

A light/dye-induced thrombosis model was used in cremaster microvessels of saline or LPS-injected mice (wild-type, P-selectin-deficient, vWF-deficient, or littermate controls). In each strain except vWF-deficient mice, LPS enhanced thrombosis in venules, resulting in approximately 30% to 55% reduction in times to thrombotic occlusion. LPS had no effect on thrombosis in vWF-deficient mice, although these mice had similar systemic responses to LPS (tachycardia, thrombocytopenia, and plasma coagulation markers). vWF-deficient mice demonstrated prolonged times to thrombotic occlusion relative to littermates. LPS increased plasma vWF in each strain studied. While immunofluorescence in wild-type mice failed to detect LPS-induced differences in microvascular vWF expression, it revealed markedly higher vWF expression in venules relative to arterioles.

CONCLUSIONS

vWF mediates light/dye-induced microvascular thrombosis and endotoxin-induced enhancement of thrombosis in mouse cremaster venules; P-selectin is not required for enhanced thrombosis in response to endotoxin. Enhanced vWF expression in venules relative to arterioles has potential implications for the differences in thrombotic responses among these microvessels.

摘要

目的

内毒素（脂多糖[LPS]）可增强小鼠提睾肌微静脉中的微血管血栓形成。由于血管性血友病因子（vWF）和P-选择素被认为介导LPS诱导的血小板-微血管相互作用，我们确定vWF和P-选择素是否在内毒素血症中促成微血管血栓形成。

方法与结果

在注射生理盐水或LPS的小鼠（野生型、P-选择素缺陷型、vWF缺陷型或同窝对照）的提睾肌微血管中使用光/染料诱导的血栓形成模型。除vWF缺陷型小鼠外，在每种品系中，LPS均增强了微静脉中的血栓形成，导致血栓闭塞时间缩短约30%至55%。LPS对vWF缺陷型小鼠的血栓形成无影响，尽管这些小鼠对LPS有相似的全身反应（心动过速、血小板减少和血浆凝血标志物）。与同窝对照相比，vWF缺陷型小鼠的血栓闭塞时间延长。LPS使所研究的每种品系的血浆vWF升高。虽然野生型小鼠的免疫荧光未检测到LPS诱导的微血管vWF表达差异，但显示微静脉中的vWF表达明显高于小动脉。

结论

vWF介导光/染料诱导的小鼠提睾肌微静脉微血管血栓形成以及内毒素诱导的血栓形成增强；内毒素诱导的血栓形成增强不需要P-选择素。与小动脉相比，微静脉中vWF表达增强对这些微血管血栓形成反应的差异具有潜在影响。

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