持续输注前列环素可使原发性肺动脉高压患者内皮细胞损伤和血小板聚集的血浆标志物恢复正常。

Continuous infusion of prostacyclin normalizes plasma markers of endothelial cell injury and platelet aggregation in primary pulmonary hypertension.

作者信息

Friedman R, Mears J G, Barst R J

机构信息

Department of Pediatrics, Columbia University College of Physicians & Surgeons, New York, NY 10032, USA.

出版信息

Circulation. 1997 Nov 4;96(9):2782-4. doi: 10.1161/01.cir.96.9.2782.

DOI:10.1161/01.cir.96.9.2782

PMID:9386137

Abstract

BACKGROUND

Primary pulmonary hypertension (PPH) is characterized by vascular injury of pulmonary arterioles, in which endothelial dysfunction may play a major role. Although continuous infusion of prostacyclin (prostaglandin I2, a potent vasodilator released by vascular endothelial cells) improves the clinical status and survival in PPH, its mechanism or mechanisms of action remain unclear.

METHODS AND RESULTS

We measured endothelium-derived clotting factors and assayed platelet aggregation in 64 patients (26 adults and 38 children) with PPH before long-term PGI2 therapy. Repeat studies were performed in 42 patients (18 adults, 24 children) after one year of PGI2 therapy. At baseline, 87% of adults and 79% of children had abnormal platelet aggregation. In addition, factor VIII, von Willebrand (vW) antigen, and ristocetin cofactor levels were abnormally high in 92%, 72%, and 52%, respectively, of the adults versus 29%, 16%, and 16%, respectively, of the children (P<.005 adults versus children). With long-term PGI2, platelet aggregation normalized in 83% of the adults and 80% of the children who had platelet aggregation abnormalities at baseline (P<.01). Factor VIII, vW antigen, and ristocetin cofactor also decreased with long-term PGI2 in both groups (P<.02). The ratio of ristocetin cofactor to vW antigen, which may reflect biological activity of vW factor, increased with long-term PGI2 in adults from an abnormally low level (0.6+/-0.2) to normal level (1.10+/-0.4), and in children the ratio increased from 0.8+/-0.3 to 1.3+/-0.4 (normal, 0.8 to 1.4).

CONCLUSIONS

Alterations in the coagulation system may contribute to the pathogenesis of PPH; the normalization of these endothelial markers concomitant with improvement in hemodynamic parameters with long-term PGI2 suggests that long-term PGI2 remodels the pulmonary vascular bed with subsequent decreases in endothelial cell injury and hypercoagulability.

摘要

背景

原发性肺动脉高压（PPH）的特征是肺小动脉血管损伤，其中内皮功能障碍可能起主要作用。尽管持续输注前列环素（前列腺素I2，一种由血管内皮细胞释放的强效血管扩张剂）可改善PPH患者的临床状况并提高生存率，但其作用机制仍不清楚。

方法与结果

我们在64例（26例成人和38例儿童）PPH患者长期接受前列环素I2（PGI2）治疗前，检测了内皮源性凝血因子并测定了血小板聚集情况。在42例（18例成人，24例儿童）患者接受PGI2治疗一年后进行了重复研究。基线时，87%的成人和79%的儿童血小板聚集异常。此外，成人中分别有92%、72%和52%的因子VIII、血管性血友病因子（vW）抗原和瑞斯托霉素辅因子水平异常升高，而儿童中这一比例分别为29%、16%和16%（成人与儿童相比，P<0.005）。长期使用PGI2后，基线时血小板聚集异常的成人中83%和儿童中80%的血小板聚集恢复正常（P<0.01）。两组中，长期使用PGI2后因子VIII、vW抗原和瑞斯托霉素辅因子也均降低（P<0.02）。瑞斯托霉素辅因子与vW抗原的比值可能反映vW因子的生物活性，长期使用PGI2后，成人该比值从异常低水平（0.6±0.2）升至正常水平（1.10±0.4），儿童该比值从0.8±0.3升至1.3±0.4（正常范围为0.8至1.4）。