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内皮祖细胞调节凝血、血小板聚集,并与颈动脉内皮细胞类似,对肿瘤坏死因子产生反应。

Endothelial outgrowth cells regulate coagulation, platelet accumulation, and respond to tumor necrosis factor similar to carotid endothelial cells.

作者信息

Glynn Jeremy J, Hinds Monica T

机构信息

Department of Biomedical Engineering, Oregon Health & Science University , Portland, Oregon.

出版信息

Tissue Eng Part A. 2015 Jan;21(1-2):174-82. doi: 10.1089/ten.TEA.2014.0032. Epub 2014 Jul 31.

Abstract

Endothelial cells (ECs) are central regulators of hemostasis, inflammation, and other vascular processes. ECs have been used to cover vascular graft materials in an attempt to improve the biological integration of the grafts with the surrounding tissue. Although EC seeded grafts demonstrated improved patency, the invasive nature of EC harvest has limited the clinical translation of this technique. Endothelial outgrowth cells (EOCs) can be derived from circulating endothelial progenitor cells, which are noninvasively isolated from a peripheral blood draw. Although EOCs have been presumed to regulate hemostasis and inflammation similarly to arterial ECs, there has been limited research that directly compares EOCs to arterial ECs, particularly using pairs of donor-matched cells. This study provides a multifaceted characterization of hemostasis regulation by baboon EOCs and carotid ECs, both in the presence and absence of an inflammatory stimulus, tumor necrosis factor α (TNFα). The expression of genes involved in thrombosis and inflammation was highly similar between ECs and EOCs at a basal state and following TNFα stimulation. ECs and EOCs activated similar levels of protein C and Factor X (FX) at a basal state. Following TNFα treatment, EOCs had less of an increase in tissue factor activity than ECs. Cell-seeded expanded polytetrafluoroethylene vascular grafts demonstrated no significant differences between ECs and EOCs in platelet accumulation or fibrinogen incorporation in a baboon femoral arteriovenous shunt loop. This work demonstrates that EOCs regulate thrombus formation and respond to an inflammatory stimulus similar to ECs, and supports utilizing EOCs as a source for an autologous endothelium in tissue engineering applications.

摘要

内皮细胞(ECs)是止血、炎症及其他血管过程的核心调节因子。人们已使用内皮细胞覆盖血管移植材料,试图改善移植材料与周围组织的生物整合。尽管接种了内皮细胞的移植物显示出更好的通畅性,但获取内皮细胞的侵入性限制了该技术的临床应用。内皮祖细胞衍生的内皮祖细胞(EOCs)可从循环内皮祖细胞中获得,这些细胞可通过外周血抽取非侵入性分离。尽管人们推测内皮祖细胞与动脉内皮细胞在调节止血和炎症方面类似,但直接将内皮祖细胞与动脉内皮细胞进行比较的研究有限,尤其是使用供体匹配的细胞对。本研究对狒狒内皮祖细胞和颈动脉内皮细胞在有或无炎症刺激肿瘤坏死因子α(TNFα)情况下的止血调节进行了多方面表征。在基础状态和TNFα刺激后,参与血栓形成和炎症的基因在内皮细胞和内皮祖细胞之间的表达高度相似。在基础状态下,内皮细胞和内皮祖细胞激活的蛋白C和因子X(FX)水平相似。TNFα处理后,内皮祖细胞的组织因子活性增加幅度小于内皮细胞。在狒狒股动静脉分流环中,接种细胞的膨体聚四氟乙烯血管移植物在内皮细胞和内皮祖细胞之间的血小板聚集或纤维蛋白原掺入方面无显著差异。这项工作表明,内皮祖细胞调节血栓形成并对炎症刺激做出反应,与内皮细胞相似,并支持在组织工程应用中利用内皮祖细胞作为自体内皮的来源。

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