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实验性失血性休克对肝脏药物清除的影响。

Effect of experimental hemorrhagic shock on hepatic drug elimination.

作者信息

DiPiro J T, Hooker K D, Sherman J C, Gaines M G, Wynn J J

机构信息

University of Georgia College of Pharmacy, Augusta.

出版信息

Crit Care Med. 1992 Jun;20(6):810-5. doi: 10.1097/00003246-199206000-00019.

Abstract

OBJECTIVE

Exogenous substrates were used to measure hepatic function for the purposes of determining organ dysfunction and to evaluate the effect of experimental hemorrhagic shock with resuscitation on hepatic drug elimination.

DESIGN

Prospective, controlled, non-randomized crossover trial.

INTERVENTIONS

Eleven chronically instrumented immature swine were studied using a fixed-volume hemorrhage model (45 mL/kg blood removal over 15 mins) followed by resuscitation with lactated Ringer's solution at three times the volume of shed blood. One week before and immediately after hemorrhage and resuscitation, hepatic function markers (indocyanine green and antipyrine) were simultaneously administered intravenously.

MEASUREMENTS

Physiologic data and blood samples were collected over 12 hrs after drug administration. Drug clearances, volumes of distribution, and half-lives were determined.

MAIN RESULTS

For indocyanine green, there was no substantial change in pharmacokinetics from preshock to postshock, suggesting minimal change in hepatic blood flow. For antipyrine, clearance was decreased by 30% after shock and resuscitation (p = .05), suggesting that oxidative metabolism was acutely impaired.

CONCLUSIONS

The information indicates that hepatic oxidative drug metabolism may be impaired early after hemorrhagic shock and that dosages of drugs in this class should be carefully examined when administered to patients who have sustained injury with hemorrhagic shock.

摘要

目的

使用外源性底物来测量肝功能,以确定器官功能障碍,并评估实验性失血性休克复苏对肝脏药物清除的影响。

设计

前瞻性、对照、非随机交叉试验。

干预措施

使用固定容量出血模型(在15分钟内抽出45 mL/kg血液)对11只长期植入仪器的未成熟猪进行研究,随后用失血量3倍体积的乳酸林格氏液进行复苏。在出血和复苏前一周以及出血和复苏后立即静脉内同时给予肝功能标志物(吲哚菁绿和安替比林)。

测量

给药后12小时内收集生理数据和血样。测定药物清除率、分布容积和半衰期。

主要结果

对于吲哚菁绿,从休克前到休克后药代动力学没有实质性变化,表明肝血流量变化最小。对于安替比林,休克和复苏后清除率降低了30%(p = 0.05),表明氧化代谢受到急性损害。

结论

这些信息表明失血性休克后早期肝脏氧化药物代谢可能受损,对于遭受失血性休克损伤的患者给药时,应仔细检查这类药物的剂量。

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