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过度透析时 RANTES 血浆浓度的增加取决于肝素剂量和心血管疾病状态。

Over-dialysis plasma RANTES increase depends on heparin dose and cardiovascular disease status.

出版信息

Adv Med Sci. 2013;58(2):311-9. doi: 10.2478/ams-2013-0008.

DOI:10.2478/ams-2013-0008
PMID:23959669
Abstract

PURPOSE

The lifespan of maintenance hemodialysis patients is reduced mainly because of cardiovascular complications due to accelerated atherosclerosis and impaired angiogenesis. We aimed to compare the effect of unfractionated heparin (UFH) and enoxaparin used as anticoagulants during hemodialysis (HD) on circulating levels of heparin-binding, anti-angiogenic Endostatin, pro-inflammatory RANTES (Regulated upon Activation, Normal T cell Expressed and Secreted), and MCP-1 (Monocyte Chemoattractant Protein-1).

METHODS

We enrolled 22 chronic HD patients, who were randomly assigned to either enoxaparin (n=11) or UFH (n=11) anticoagulation, and followed prospectively for 12 weeks before crossing over to the alternate therapy for further 12 weeks. The factors were measured (ELISA) at the start, 10 and 180 min of HD, and compared to 20 healthy volunteers.

RESULTS

The baseline Endostatin, RANTES, and MCP-1 levels in patients were higher than in controls and comparable during enoxaparin and UFH treatment. RANTES significantly increased during both enoxaparin and UFH anticoagulated HD, while over-HD Endostatin and MCP-1 levels remained stable regardless of the heparin sort. About 25% RANTES increase after 10 min of HD positively correlated with the dose of both heparins and HD duration. The switch from enoxaparin to UFH treatment had no impact on the levels of parameters studied. Patients with ischemic heart disease had less RANTES increase after 180 min of HD especially during enoxaparin treatment.

CONCLUSION

RANTES is dose-depended and transitory increased in response to both UFH and enoxaparin administration during HD. Cardiovascular disease status occurred to be the most important predictor of its over-HD level.

摘要

目的

维持性血液透析患者的寿命缩短主要是由于心血管并发症导致的加速动脉粥样硬化和血管生成受损。我们旨在比较在血液透析(HD)中使用未分馏肝素(UFH)和依诺肝素作为抗凝剂对循环中肝素结合的、抗血管生成的内皮抑素、促炎的 RANTES(活化正常 T 细胞表达和分泌)和单核细胞趋化蛋白-1(MCP-1)水平的影响。

方法

我们纳入了 22 例慢性 HD 患者,他们被随机分配到依诺肝素(n=11)或 UFH(n=11)抗凝组,并前瞻性随访 12 周,然后交叉到另一种治疗方案再随访 12 周。在 HD 开始、10 和 180 分钟时测量这些因素(ELISA),并与 20 名健康志愿者进行比较。

结果

患者的基线内皮抑素、RANTES 和 MCP-1 水平高于对照组,并且在依诺肝素和 UFH 治疗期间相当。在依诺肝素和 UFH 抗凝的 HD 期间,RANTES 明显增加,而超 HD 内皮抑素和 MCP-1 水平保持稳定,与肝素种类无关。HD 开始后 10 分钟内 RANTES 增加约 25%,与两种肝素的剂量和 HD 持续时间呈正相关。从依诺肝素切换到 UFH 治疗对研究的参数水平没有影响。缺血性心脏病患者在 HD 180 分钟后 RANTES 增加较少,特别是在依诺肝素治疗期间。

结论

在 HD 期间,UFH 和依诺肝素给药会引起 RANTES 剂量依赖性和短暂增加。心血管疾病状态是其超 HD 水平的最重要预测因素。

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