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体外循环中肝素与鱼精蛋白应用的安全问题

Safety issues in heparin and protamine administration for extracorporeal circulation.

作者信息

Jobes D R

机构信息

Department of Anesthesia, University of Pennsylvania School of Medicine, and The Children's Hospital of Philadelphia, USA.

出版信息

J Cardiothorac Vasc Anesth. 1998 Apr;12(2 Suppl 1):17-20.

PMID:9583571
Abstract

This article reviews past approaches to heparin and protamine dosing and summarizes current practice. The author elucidates his experience with the Celite activated coagulation time (ACT), with attention to his adoption of a value of 400 seconds for this time; the adoption of an ACT of 480 seconds by Bull et al (J Thorac Cardiovasc Surg 69:674-684, 1975) and Young et al (Ann Thorac Surg 26:231-240, 1978); the proposed use of heparin response curves by Bull et al; the author's experience with a unitized dosing system to individualize dosing of heparin; and the use for this purpose by Despotis et al (J Thorac Cardiovasc Surg 110:46-54, 1995) of a system based on protamine titration. In more than 270 adult cardiac surgery patients, the unitized dosing system identified patients with high sensitivity or resistance to heparin and facilitated exact individualized doses to be given to produce the desired effect. Thus, less heparin was used in short bypass runs. Patients received less protamine than they would have with any other formula, and there was less blood loss and fewer transfusions required. Currently, no claims for efficacy or safety can be made for maintaining heparin concentrations greater than 3 U/mL. Pending further clarification, heparin dosage cannot be safely reduced when using heparin-bonded circuits. Aprotinin is not a procoagulant during cardiopulmonary bypass. Emerging studies suggest that graft patency is not affected by aprotinin use. The Celite ACT should not be used to monitor heparin effect and safety when using aprotinin; the kaolin ACT should be used instead.

摘要

本文回顾了过去肝素和鱼精蛋白给药的方法,并总结了当前的实践。作者阐述了他使用硅藻土激活凝血时间(ACT)的经验,尤其关注他采用400秒作为该时间值的情况;Bull等人(《胸心血管外科杂志》69:674 - 684, 1975年)和Young等人(《胸外科年鉴》26:231 - 240, 1978年)采用480秒的ACT;Bull等人提议使用肝素反应曲线;作者使用单位剂量给药系统个体化肝素给药的经验;以及Despotis等人(《胸心血管外科杂志》110:46 - 54, 1995年)基于鱼精蛋白滴定的系统用于此目的的情况。在超过270例成年心脏手术患者中,单位剂量给药系统识别出对肝素高敏或耐药的患者,并有助于给予精确的个体化剂量以产生预期效果。因此,在短体外循环时间中使用的肝素较少。患者接受的鱼精蛋白比使用任何其他配方时都少,失血更少,所需输血也更少。目前,对于维持肝素浓度大于3 U/mL,无法提出疗效或安全性的主张。在进一步明确之前,使用肝素涂层回路时不能安全地降低肝素剂量。抑肽酶在体外循环期间不是促凝剂。新出现的研究表明,使用抑肽酶不影响移植物通畅率。使用抑肽酶时,不应使用硅藻土ACT来监测肝素的效果和安全性;而应使用高岭土ACT。

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