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一种一氧化氮释放聚合物对兔体外循环模型中血小板和单核细胞活化的抑制作用。

The attenuation of platelet and monocyte activation in a rabbit model of extracorporeal circulation by a nitric oxide releasing polymer.

机构信息

Department of Surgery, University of Michigan Medical Center, Ann Arbor, MI 48109, USA.

出版信息

Biomaterials. 2010 Apr;31(10):2736-45. doi: 10.1016/j.biomaterials.2009.12.028. Epub 2009 Dec 29.

Abstract

Nitric oxide (NO) has been shown to reduce thrombogenicity by decreasing platelet and monocyte activation by the surface glycoprotein, P-selectin and the integrin, CD11b, respectively. In order to prevent platelet and monocyte activation with exposure to an extracorporeal circulation (ECC), a nitric oxide releasing (NORel) polymeric coating composed of plasticized polyvinyl chloride (PVC) blended with a lipophilic N-diazeniumdiolate was evaluated in a 4 h rabbit thrombogenicity model using flow cytometry. The NORel polymer significantly reduced ECC thrombus formation compared to polymer control after 4 h blood exposure (2.8 +/- 0.7 NORel vs 6.7 +/- 0.4 pixels/cm(2) control). Platelet count (3.4 +/- 0.3 NORel vs 2.3 +/- 0.3 x 10(8)/ml control) and function as measured by aggregometry (71 +/- 3 NORel vs 17 +/- 6% control) were preserved after 4 h exposure in NORel versus control ECC. Plasma fibrinogen levels significantly decreased in both NORel and control groups. Platelet P-selectin mean fluorescence intensity (MFI) as measured by flow cytometry was attenuated after 4 h on ECC to ex vivo collagen stimulation (27 +/- 1 NORel vs 40 +/- 2 MFI control). Monocyte CD11b expression was reduced after 4 h on ECC with NORel polymer (87 +/- 14 NORel vs 162 +/- 30 MFI control). These results suggest that the NORel polymer coatings attenuate the increase in both platelet P-selectin and monocytic CD11b integrin expression in blood exposure to ECCs. These NO-mediated platelet and monocytic changes were shown to improve thromboresistance of these NORel-polymer-coated ECCs for biomedical devices.

摘要

一氧化氮 (NO) 已被证明可通过分别降低血小板和单核细胞表面糖蛋白 P-选择素和整合素 CD11b 的活性来降低血栓形成性。为了防止暴露于体外循环 (ECC) 时血小板和单核细胞的激活,使用流式细胞术在 4 小时兔血栓形成模型中评估了由增塑聚氯乙烯 (PVC) 与亲脂性 N-二氮烯二醇混合组成的一氧化氮释放 (NORel) 聚合物涂层。与聚合物对照相比,NORel 聚合物在 4 小时血液暴露后显著减少 ECC 血栓形成(2.8 +/- 0.7 NORel 与 6.7 +/- 0.4 像素/cm(2) 对照)。与对照 ECC 相比,NORel 中血小板计数(3.4 +/- 0.3 NORel 与 2.3 +/- 0.3 x 10(8)/ml 对照)和通过聚集测定法测量的功能(71 +/- 3 NORel 与 17 +/- 6% 对照)在 4 小时暴露后得以保留。NORel 和对照组的血浆纤维蛋白原水平均显著降低。用流式细胞术测量的血小板 P-选择素平均荧光强度 (MFI) 在 ECC 上 4 小时后在体外胶原蛋白刺激下减弱(27 +/- 1 NORel 与 40 +/- 2 MFI 对照)。NORel 聚合物上的单核细胞 CD11b 表达在 4 小时 ECC 后减少(87 +/- 14 NORel 与 162 +/- 30 MFI 对照)。这些结果表明,NORel 聚合物涂层可减轻暴露于 ECC 血液中血小板 P-选择素和单核细胞 CD11b 整合素表达的增加。这些 NO 介导的血小板和单核细胞变化表明,这些 NORel 聚合物涂层的 ECC 的抗血栓性得到了改善,适用于生物医学设备。

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