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组织因子、血栓调节蛋白和E选择素在患有致死性大肠杆菌败血症的狒狒中的表达

Expression of tissue factor, thrombomodulin, and E-selectin in baboons with lethal Escherichia coli sepsis.

作者信息

Drake T A, Cheng J, Chang A, Taylor F B

机构信息

Department of Pathology and Laboratory Medicine, UCLA 90024-1732.

出版信息

Am J Pathol. 1993 May;142(5):1458-70.

Abstract

Disseminated intravascular thrombosis is a frequent complication of endotoxic shock, and modulation of endothelial cell hemostatic properties has been proposed to play a role in its pathogenesis based on studies of endothelial cells in culture. This study examined the in vivo expression of tissue factor (TF) and thrombomodulin (TM) in a baboon model of lethal Escherichia coli sepsis using immunohistochemistry with monospecific antibodies. Expression of E-selectin (E-sel) was also determined as a marker of endothelial cell activation. Correlation of immunoreactivity with procoagulant activity in lipopolysaccharide-stimulated cultured human endothelial cells showed that immunohistochemistry was sufficiently sensitive to detect as little as 5% of the maximum in vitro endothelial cell TF response. Vascular endothelium of control animals expressed TM but had no detectable TF or E-sel. Following E. coli infusion, widespread E-sel expression and microvascular fibrin deposition was evident within 6 hours. However, expression of TF by endothelial cells became detectable only in the splenic microvasculature, where endothelial specificity of TF expression was confirmed by dual immunofluorescence of TF with von Willebrand's factor and with TM. In the spleen, there was a dissociation of expression of TF and E-sel, with marginal zone vessels being TF-positive and E-sel-negative, whereas sinusoidal endothelium was E-sel-positive but TF-negative. TM expression was unchanged from controls. Additionally, expression of TF by lung alveolar epithelial cells, splenic macrophages, and epithelial cells of the renal glomeruli was observed to be enhanced in septic animals. This study documents endothelial cell expression of TF in vivo in a relevant pathological setting. At the same time, compared with endothelial cells in culture, there is in vivo both significantly greater control of TF expression than expected, given the strong positive stimuli present in lethal E. coli septic shock and an unpredicted heterogeneity of activation responses.

摘要

弥散性血管内血栓形成是内毒素休克常见的并发症,基于对培养内皮细胞的研究,有人提出内皮细胞止血特性的调节在其发病机制中起作用。本研究使用单特异性抗体免疫组织化学方法,检测了致死性大肠杆菌败血症狒狒模型中组织因子(TF)和血栓调节蛋白(TM)的体内表达。还测定了E-选择素(E-sel)的表达作为内皮细胞活化的标志物。免疫反应性与脂多糖刺激的培养人内皮细胞促凝活性的相关性表明,免疫组织化学足够灵敏,能够检测到低至体外内皮细胞TF最大反应5%的水平。对照动物的血管内皮表达TM,但未检测到TF或E-sel。注入大肠杆菌后,6小时内可见广泛的E-sel表达和微血管纤维蛋白沉积。然而,内皮细胞TF的表达仅在脾微血管中可检测到,通过TF与血管性血友病因子及TM的双重免疫荧光证实了TF表达的内皮特异性。在脾脏中,TF和E-sel的表达存在分离,边缘区血管TF阳性而E-sel阴性,而窦状内皮E-sel阳性但TF阴性。TM表达与对照无变化。此外,观察到脓毒症动物肺肺泡上皮细胞、脾巨噬细胞和肾小球上皮细胞中TF的表达增强。本研究记录了在相关病理环境中TF在体内的内皮细胞表达。同时,与培养的内皮细胞相比,在体内,尽管致死性大肠杆菌败血症休克中存在强烈的阳性刺激,但TF表达的控制明显强于预期,且活化反应存在不可预测的异质性。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/0ce5/1886910/cd52341e8b5f/amjpathol00077-0138-a.jpg

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