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自发性血纤维蛋白塞肺栓塞微创模型在 Sprague-Dawley 和 Copenhagen 大鼠中的建立与比较。

Development and comparison of a minimally-invasive model of autologous clot pulmonary embolism in Sprague-Dawley and Copenhagen rats.

机构信息

Emergency Medicine Research, Carolinas Medical Center, Charlotte, NC, USA.

出版信息

Thromb J. 2010 Feb 11;8:3. doi: 10.1186/1477-9560-8-3.

Abstract

BACKGROUND

Experimental models of pulmonary embolism (PE) that produce pulmonary hypertension (PH) employ many different methods of inducing acute pulmonary occlusion. Many of these models induce PE with intravenous injection of exogenous impervious objects that may not completely reproduce the physiological properties of autologous thromboembolism. Current literature lacks a simple, well-described rat model of autlogous PE.

OBJECTIVE

Test if moderate-severity autologous PE in Sprague-Dawley (SD) and Copenhagen (Cop) rats can produce persistent PH.

METHODS

blood was withdrawn from the jugular vein, treated with thrombin-Ca++ and re-injected following pretreatment with tranexamic acid. Hemodynamic values, clot weights and biochemical measurements were performed at 1 and 5 days.

RESULTS

Infusion of clot significantly increased the right ventricular peak systolic pressure to 45-55 mm Hg, followed by normalization within 24 hours in SD rats, and within 5 days in COP rats. Clot lysis was 95% (24 hours) and 97% (5 days) in SD rats and was significantly lower in COP rats (70%, 24 hours; 87% 5 days). Plasma D-dimer was elevated in surgical sham animals and was further increased 8 hours after pulmonary embolism. Neither strain showed a significant increase in bronchoalveolar chemotactic activity, myeloperoxidase activity, leukocyte infiltration, or chemokine accumulation, indicating that there was no significant pulmonary inflammation.

CONCLUSIONS

Both SD and COP rats exhibited near complete fibrinolysis of autologous clot PE within 5 days. Neither strain developed persistent PH. Experimental models of PE designed to induce sustained PH and a robust inflammatory response appear to require significant, persistent pulmonary vascular occlusion.

摘要

背景

产生肺动脉高压(PH)的肺栓塞(PE)实验模型采用了许多不同的方法来诱发急性肺闭塞。这些模型中的许多都是通过静脉内注射外来的不透水物体来诱发 PE,而这些物体可能无法完全再现自体血栓栓塞的生理特性。目前的文献缺乏一种简单、描述良好的自体 PE 大鼠模型。

目的

测试 Sprague-Dawley(SD)和哥本哈根(Cop)大鼠中度严重的自体 PE 是否能产生持续的 PH。

方法

从颈静脉抽取血液,用凝血酶-Ca++处理,并用氨甲环酸预处理后再注入。在第 1 天和第 5 天进行血流动力学值、凝块重量和生化测量。

结果

注入凝块后,右心室收缩峰压显著升高至 45-55mmHg,SD 大鼠在 24 小时内恢复正常,COP 大鼠在 5 天内恢复正常。SD 大鼠的凝块溶解率为 95%(24 小时)和 97%(5 天),COP 大鼠的溶解率明显较低(24 小时为 70%,5 天为 87%)。手术假手术动物的血浆 D-二聚体升高,在肺栓塞后 8 小时进一步升高。两种大鼠均未出现明显的支气管肺泡趋化活性、髓过氧化物酶活性、白细胞浸润或趋化因子积聚增加,表明没有明显的肺炎症。

结论

SD 和 COP 大鼠的自体血凝块 PE 在 5 天内几乎完全溶解。两种大鼠均未发展为持续性 PH。设计用于诱导持续 PH 和强烈炎症反应的 PE 实验模型似乎需要显著的、持续的肺血管闭塞。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/f765/2843658/3e1a9ba5d36b/1477-9560-8-3-1.jpg

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