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[阿片类药物、脑循环与颅内压]

[Opioids, cerebral circulation and intracranial pressure].

作者信息

Schregel W, Weyerer W, Cunitz G

机构信息

Klinik für Anaesthesie und operative Intensivtherapie, Knappschaftskrankenhaus, Ruhr-Universität Bochum RUB.

出版信息

Anaesthesist. 1994 Jul;43(7):421-30. doi: 10.1007/s001010050074.

Abstract

The effects of the opioids alfentanil (A), fentanyl (F), and sufentanil (S) on cerebral blood flow (CBF) and intracranial pressure (ICP) have been discussed in several recent publications. The purpose of this review is to describe the results of studies in animals, healthy volunteers, and patients with and without intracranial diseases. Clinical relevance and mechanisms of the reported ICP and CBF increases are analysed. METHODS. Approximately 70 original articles and abstracts were retrieved by a systematic literature search using the key word list at the end of this abstract. The cited studies came from computerised database systems like Silver Platter and DIMDI, the SNACC reference list, and the bibliographies of pertinent articles and books. These studies were classified into three groups: significant increase of ICP and/or CBF; no significant or clinically relevant alterations; and significant decreases of ICP and/or CBF. RESULTS. The numerical relationship was 6:7:3 for A, 7:16:9 for F, and 5:11:8 for S. Increases of previously normal or only slightly elevated ICP were registered in some studies in connection with a decrease in mean arterial pressure (MAP). On the other hand, in patients with brain injury and elevated ICP opioids did not further increase ICP despite MAP decreases. In studies monitoring ICP and/or CBF continuously, transient and moderate increases of questionable clinical relevance became apparent a few minutes after bolus injection of opioids. Alterations of systemic and cerebral haemodynamics observed after bolus application were not registered during continuous infusion of A and S. DISCUSSION AND CONCLUSIONS. The cerebral effects of opioids are dependent on several factors, e.g., age, species, ventilation, anaesthesia before and during measurements, systemic haemodynamics, and underlying diseases. The probable mechanism of ICP increase during decreasing MAP is cerebral vasodilatation due to maintained autoregulation. With increasing severity of the cerebral lesion autoregulation is often disturbed. Therefore, ICP often remains unaltered despite MAP decreases. However, the resulting decrease in cerebral perfusion pressure makes such patients more susceptible to develop ischaemic neurological deficits. Induction of somatic rigidity or (with high doses) convulsions, exceeding the upper limit of autoregulation, histamine release, cerebral vasodilatation, increased cerebral oxygen consumption, or carbon dioxide accumulation during spontaneous breathing were discussed as mechanisms for transient ICP/CBF increases. It is concluded that opioids are often beneficial and not generally contraindicated for patients with cerebral diseases and compromised intracranial compliance. However, since negative side effects cannot be excluded, opioid effects and side effects should be monitored (MAP, ICP, cerebrovenous oxygen saturation, transcranial Doppler sonography) in patients at risk. It has to be stressed that opioids should be administered only to patients with stable haemodynamic situations and preferably in well-titrated, continuous infusions.

摘要

近期有几篇出版物讨论了阿芬太尼(A)、芬太尼(F)和舒芬太尼(S)等阿片类药物对脑血流量(CBF)和颅内压(ICP)的影响。本综述的目的是描述在动物、健康志愿者以及有无颅内疾病患者中开展的研究结果。分析所报道的ICP和CBF升高的临床相关性及机制。方法:通过使用本摘要末尾的关键词列表进行系统的文献检索,检索到约70篇原始文章和摘要。引用的研究来自Silver Platter和DIMDI等计算机化数据库系统、SNACC参考文献列表以及相关文章和书籍的参考文献。这些研究分为三组:ICP和/或CBF显著升高;无显著或临床相关改变;ICP和/或CBF显著降低。结果:A组的数字关系为6:7:3,F组为7:16:9,S组为5:11:8。在一些研究中,先前正常或仅轻度升高的ICP升高与平均动脉压(MAP)降低有关。另一方面,在脑损伤且ICP升高的患者中,尽管MAP降低,阿片类药物并未进一步升高ICP。在持续监测ICP和/或CBF的研究中,推注阿片类药物几分钟后出现了具有可疑临床相关性的短暂中度升高。推注后观察到的全身和脑血流动力学改变在持续输注A和S期间未出现。讨论与结论:阿片类药物对脑的影响取决于几个因素,例如年龄、物种、通气、测量前和测量期间的麻醉、全身血流动力学以及基础疾病。MAP降低期间ICP升高的可能机制是由于自动调节维持导致脑血管扩张。随着脑损伤严重程度的增加,自动调节常常受到干扰。因此,尽管MAP降低,ICP通常保持不变。然而,由此导致的脑灌注压降低使此类患者更容易出现缺血性神经功能缺损。躯体强直的诱发或(高剂量时)惊厥、超过自动调节上限、组胺释放、脑血管扩张、脑氧消耗增加或自主呼吸期间二氧化碳蓄积被讨论为ICP/CBF短暂升高的机制。得出的结论是,阿片类药物通常对患有脑部疾病和颅内顺应性受损的患者有益,一般并非禁忌。然而,由于不能排除负面副作用,对于有风险的患者应监测阿片类药物的作用和副作用(MAP、ICP、脑静脉血氧饱和度、经颅多普勒超声)。必须强调的是,阿片类药物仅应给予血流动力学稳定的患者,并且最好采用滴定良好的持续输注方式给药。

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