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肝素与前列环素在连续性血液透析滤过治疗急性肾衰竭中的比较:对全身循环和滤器中血小板功能的影响。

Heparin versus prostacyclin in continuous hemodiafiltration for acute renal failure: effects on platelet function in the systemic circulation and across the filter.

机构信息

Istituto Anestesia e Rianimazione, Policlinico Agostino Gemelli, Catholic University School of Medicine, Largo Francesco Vito 1, 00168 Rome, Italy.

出版信息

Thromb Res. 2010 Jul;126(1):24-31. doi: 10.1016/j.thromres.2010.01.048. Epub 2010 Feb 24.

DOI:10.1016/j.thromres.2010.01.048
PMID:20185164
Abstract

Continuous venovenous hemodiafiltration (CVVHDF) is the treatment of choice for critically-ill patients suffering from acute renal failure (ARF). One major problem of extracorporeal circuits is their thrombogenicity, which requires pharmacological blockade of primary (platelet-dependent) or secondary (plasmatic) haemostasis, increasing the patient's bleeding risk. Our study assessed platelet function during CVVHDF, comparing anticoagulant versus antiplatelet pharmacological strategies, commonly used to avoid circuit clotting. Twenty-three critically-ill patients with ARF, requiring CVVHDF were randomized to a prostacyclin analogue (PGI) or to unfractionated heparin (UFH). Ex vivo platelet function, assessed by optical aggregometry (OPA) induced by collagen or ADP, was studied in peripheral blood at baseline, 4 and 24 hrs after starting CVVHDF, and at 4 hrs within the circuit, before and after the filter (n=9). Coagulation was also monitored. PGI significantly inhibited ADP-induced OPA of peripheral platelets: maximal aggregation (Tmax) was reduced at 4 and 24 hrs by 20%, while collagen-induced Tmax was significantly reduced at 4 hrs only. In the UFH group, collagen-induced OPA in peripheral platelets was significantly inhibited: slopes of OPA tracings were decreased by 25%, lag time was prolonged by 22%, Tmax decreased by 10% already at 4 hrs. ADP-induced OPA showed a similar, but non-significant trend. UFH expectedly prolonged aPTT. In the UFH group, platelet responsiveness to collagen was significantly increased by 30% in post-filter versus pre-filter samples. This effect was blunted in the PGI group. UFH does not protect platelets from filter-induced activation and is associated with a reduced function of systemic platelets. Platelet-inhibiting agents might better prevent the activatory effect of the filter.

摘要

连续静脉-静脉血液透析滤过(CVVHDF)是治疗急性肾衰竭(ARF)危重症患者的首选方法。体外回路的一个主要问题是其血栓形成性,这需要药理学阻断原发性(血小板依赖性)或继发性(血浆)止血,增加患者的出血风险。我们的研究评估了 CVVHDF 过程中的血小板功能,比较了抗凝与抗血小板药理学策略,这些策略常用于避免回路凝血。23 名 ARF 危重症患者需要 CVVHDF,随机分为前列环素类似物(PGI)或未分级肝素(UFH)组。通过光学聚集仪(OPA)评估体外诱导的胶原或 ADP 诱导的血小板功能,在基线、开始 CVVHDF 后 4 小时和 24 小时以及在回路中 4 小时(n=9)时进行外周血研究,在过滤器前后。还监测了凝血情况。PGI 显著抑制 ADP 诱导的外周血小板 OPA:最大聚集(Tmax)在 4 小时和 24 小时分别减少 20%,而胶原诱导的 Tmax 在仅 4 小时显著减少。在 UFH 组中,胶原诱导的外周血小板 OPA 显著抑制:OPA 轨迹斜率降低 25%,延迟时间延长 22%,Tmax 在 4 小时时已经降低 10%。ADP 诱导的 OPA 显示出相似但无统计学意义的趋势。UFH 预期地延长了 aPTT。在 UFH 组中,与过滤前样本相比,过滤后样本中胶原诱导的 OPA 血小板反应性增加了 30%。在 PGI 组中,这种作用减弱。UFH 不能保护血小板免受过滤器引起的激活,并且与全身血小板功能降低有关。血小板抑制剂可能更好地预防过滤器的激活作用。

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