Davis P J, Cook D R
Clin Pharmacokinet. 1986 Jan-Feb;11(1):18-35. doi: 10.2165/00003088-198611010-00002.
In the last 15 years the role of opioids in anaesthesia management has undergone dramatic change. Initially used as premedicants, or adjuvants to inhalation anaesthetic agents or as analgesics for postoperative pain relief, narcotics have now evolved into primary anaesthetic agents, primarily because of their ability to maintain cardiovascular stability especially in patients with compromised myocardial function. Sufentanil, alfentanil, and lofentanil are 3 new synthetic congeners of fentanyl. Sufentanil and alfentanil afford not only the haemodynamic stability but also the desirable anaesthetic properties of analgesia, and unconsciousness. Their major advantage lies in their pharmacokinetic behaviour; a rapid onset of action and short elimination half-life, allowing for greater flexibility in anaesthetic management. Sufentanil's pharmacokinetic profile is consistent with a 2-compartment model. Its elimination half-life is 149 minutes and its clearance is 11.3 ml/min/kg. Alfentanil's pharmacokinetic profile has been described by both 2- and 3-compartment models. Its distribution and redistribution are rapid, with an elimination half-life of 83 to 137 minutes and a clearance of 4.37 to 6.47 ml/min/kg in adult patients. Lofentanil, however, is an extremely long-acting narcotic analgesic. Presently, its use is justified only when prolonged mechanical ventilation is anticipated. Etomidate, a carboxylated imidazole, is rapidly distributed within a central compartment and then to peripheral compartments; its slow distribution and terminal elimination half-lives are 28 and 273 to 330 minutes, respectively, and its clearance (11.6 to 25 ml/min/kg) is equal to its hepatic plasma flow. Its ability to maintain cardiovascular stability in patients with compromised myocardial function make it a useful induction agent. However, reports of increased mortality and inhibition of steroidogenesis in patients receiving either single injections or constant infusions have created controversies regarding its use. Minaxolone is a water-soluble steroid whose pharmacokinetic profile is consistent with a 2-compartment model. Distribution is rapid with a mean half-life of 2.1 minutes and an elimination half-life of 47 minutes. There do not appear to be any cumulative effects. Plasma levels on recovery were similar in those patients receiving single bolus or continuous infusions. Midazolam and flunitrazepam are two new benzodiazepines. As a class of drugs, benzodiazepines provide the pharmacological properties of anxiolysis, sedation, hypnosis, muscle relaxation, amnesia and anticonvulsant activity.(ABSTRACT TRUNCATED AT 400 WORDS)
在过去15年中,阿片类药物在麻醉管理中的作用发生了巨大变化。最初用作术前用药、吸入麻醉剂的辅助药物或术后镇痛的镇痛药,如今麻醉药已演变为主要麻醉剂,主要是因为它们能够维持心血管稳定性,尤其是在心肌功能受损的患者中。舒芬太尼、阿芬太尼和洛芬太尼是芬太尼的3种新的合成同系物。舒芬太尼和阿芬太尼不仅能提供血流动力学稳定性,还具有理想的镇痛和麻醉特性,即意识丧失。它们的主要优势在于其药代动力学行为;起效迅速且消除半衰期短,这使得麻醉管理具有更大的灵活性。舒芬太尼的药代动力学特征符合二室模型。其消除半衰期为149分钟,清除率为11.3毫升/分钟/千克。阿芬太尼的药代动力学特征已由二室和三室模型描述。其分布和再分布迅速,成年患者的消除半衰期为83至137分钟,清除率为4.37至6.47毫升/分钟/千克。然而,洛芬太尼是一种作用极长的麻醉性镇痛药。目前,仅在预计需要长时间机械通气时才证明其使用合理。依托咪酯是一种羧化咪唑,在中央室迅速分布,然后再分布到外周室;其缓慢分布和终末消除半衰期分别为28分钟和273至330分钟,其清除率(11.6至25毫升/分钟/千克)等于肝血浆流量。它在心肌功能受损患者中维持心血管稳定性的能力使其成为一种有用的诱导剂。然而,关于单次注射或持续输注依托咪酯的患者死亡率增加和类固醇生成受抑制的报道引发了关于其使用的争议。米那索龙是一种水溶性类固醇,其药代动力学特征符合二室模型。分布迅速,平均半衰期为2.1分钟,消除半衰期为47分钟。似乎没有任何累积效应。接受单次推注或持续输注的患者恢复时的血浆水平相似。咪达唑仑和氟硝西泮是两种新型苯二氮䓬类药物。作为一类药物,苯二氮䓬类药物具有抗焦虑、镇静、催眠、肌肉松弛、遗忘和抗惊厥活性等药理特性。(摘要截选至400字)
