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阿芬太尼的药效学。血浆蛋白结合的作用。

Pharmacodynamics of alfentanil. The role of plasma protein binding.

作者信息

Lemmens H J, Burm A G, Bovill J G, Hennis P J, Gladines M P

机构信息

Department of Anesthesiology, Leiden University Hospital, The Netherlands.

出版信息

Anesthesiology. 1992 Jan;76(1):65-70. doi: 10.1097/00000542-199201000-00010.

Abstract

The role of protein binding in relation to the pharmacodynamics of alfentanil was investigated in 15 female and 13 male patients, aged 21-85 yr, ASA physical status 1 or 2, undergoing upper abdominal surgery. All patients had normal cardiac, hepatic, renal, and pulmonary function. None was receiving medication or had a history of alcohol or other drug abuse. Anesthesia was induced and maintained with 66% nitrous oxide in oxygen and alfentanil. Alfentanil was administered by a computer-controlled infusion pump. If, during surgery, the patient exhibited signs of inadequate anesthesia (i.e., response), the target alfentanil plasma concentration was increased by 50-100 ng/ml. If there was no response during a 15-min period, the target concentration was decreased by 50-100 ng/ml. Arterial blood samples were taken before any change of the target concentration and 4 min after the computer had indicated that the new target concentration had been reached. In addition, blood samples were taken before intubation, skin incision, and in the patients in whom ventilation recovered spontaneously before extubation. In the remaining patients a blood sample was taken before the administration of naloxone. Plasma alfentanil concentrations were determined by capillary gas chromatography. Alfentanil protein binding was determined by equilibrium dialysis in an arterial blood sample taken before induction of anesthesia. Alfentanil concentration-effect data were evaluated by logistic regression, where effect was either response or no response to perioperative stimuli. The average free fraction of alfentanil was 9.3 +/- 3.9% (range 3.7-19.1%). For intubation, skin incision, and postanesthesia ventilation, it was not possible to characterize the concentration-effect curves based on total plasma concentrations with logistic regression.(ABSTRACT TRUNCATED AT 250 WORDS)

摘要

在15名女性和13名男性患者(年龄21 - 85岁,美国麻醉医师协会身体状况分级为1或2级)中研究了蛋白结合在阿芬太尼药效学中的作用,这些患者均接受上腹部手术。所有患者心脏、肝脏、肾脏和肺功能正常。无人正在接受药物治疗,也无酒精或其他药物滥用史。麻醉诱导和维持采用66%氧化亚氮 - 氧气混合气体及阿芬太尼。阿芬太尼通过计算机控制的输注泵给药。手术期间,如果患者出现麻醉不足的迹象(即有反应),目标阿芬太尼血浆浓度增加50 - 100 ng/ml。如果在15分钟内无反应,目标浓度降低50 - 100 ng/ml。在目标浓度改变前及计算机显示新目标浓度达到后4分钟采集动脉血样本。此外,在插管前、皮肤切开时以及拔管前自主恢复通气的患者中采集血样本。其余患者在给予纳洛酮前采集血样本。血浆阿芬太尼浓度通过毛细管气相色谱法测定。阿芬太尼蛋白结合通过麻醉诱导前采集的动脉血样本经平衡透析测定。阿芬太尼浓度 - 效应数据采用逻辑回归进行评估,效应为对围手术期刺激有反应或无反应。阿芬太尼的平均游离分数为9.3±3.9%(范围3.7 - 19.1%)。对于插管、皮肤切开和麻醉后通气,基于总血浆浓度采用逻辑回归无法描绘浓度 - 效应曲线。(摘要截断于250字)

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