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依托咪酯对灵长类动物体感和经颅磁刺激诱发的脊髓运动诱发电位的剂量反应

Etomidate dose-response on somatosensory and transcranial magnetic induced spinal motor evoked potentials in primates.

作者信息

Ghaly R F, Lee J J, Ham J H, Stone J L, George S, Raccforte P

机构信息

Chicago Institute of Neurosurgery and Neuroresearch, IL 60614, USA.

出版信息

Neurol Res. 1999 Dec;21(8):714-20. doi: 10.1080/01616412.1999.11741003.

Abstract

There is growing interest and need to monitor reliably both motor (MEP) and somatosensory (SEP) evoked potentials under anesthesia. On a pre-established primate model, the present study examined the effect of incremental etomidate (ET) dosages on spinal neural MEPs to transcranial magnetic stimulation (TMS) and posterior tibial rate (PTN) SEPs. Through a small thoracic T11-T12 laminotomy, an insulated double bipolar electrode was inserted epidurally in seven cynomolgus monkeys. Spinal TMS-MEPs, PTN-SEPs, and frontal EEG were tested against graded increase of ET doses. Etomidate 0.5 mg kg-1 i.v. was initially given and followed by 30 min continuous infusion of 0.01 mg kg-1 min-1, 0.018, 0.032, 0.056, 0.1, and 0.18 mg kg-1 min-1 in that order. Measurable spinal MEPs and SEPs were recorded under deep ET anesthesia (total 12.38 mg kg-1 cumulative dose over 180 min). The EEG showed marked slow wave and graded burst suppression at cumulative dose of > or = 3.14 mg kg-1. The direct (D) and subsequent initial indirect (I) waves (I1, I2, I3) were reproducible at doses < 0.18 mg kg-1 min-1 infusion. The latter I-waves (I4 and I5) showed graded loss at infusion dosage 0.056 mg kg-1 min-1. Etomidate remains an anesthetic of attractive features in neuroanesthesia. In the primate model, neural MEPs-SEPs were reproducible despite the exceedingly high dose of ET and markedly depressed EEG. Moreover, MEP-SEP can be monitored during ET burst-suppressive neuroprotective state. The study may set a model in humans for intra-operative multi-modality neurophysiologic recording under ET-based anesthesia.

摘要

在麻醉状态下可靠地监测运动诱发电位(MEP)和体感诱发电位(SEP)的兴趣和需求日益增加。在一个预先建立的灵长类动物模型上,本研究考察了递增剂量依托咪酯(ET)对经颅磁刺激(TMS)诱发的脊髓神经MEP以及胫后神经(PTN)SEP的影响。通过一个小的胸段T11 - T12椎板切开术,将一个绝缘的双极电极硬膜外插入7只食蟹猴体内。针对ET剂量的分级增加测试脊髓TMS - MEP、PTN - SEP和额叶脑电图。最初静脉注射0.5 mg/kg的依托咪酯,随后依次以0.01 mg·kg⁻¹·min⁻¹、0.018、0.032、0.056、0.1和0.18 mg·kg⁻¹·min⁻¹的速度持续输注30分钟。在深度ET麻醉下(180分钟内累计剂量达12.38 mg/kg)记录到了可测量的脊髓MEP和SEP。当累计剂量≥3.14 mg/kg时,脑电图显示出明显的慢波和分级爆发抑制。在输注剂量<0.18 mg·kg⁻¹·min⁻¹时,直接(D)波和随后的初始间接(I)波(I1、I2、I3)是可重复的。在输注剂量为0.056 mg·kg⁻¹·min⁻¹时,后一组I波(I4和I5)显示出分级性消失。依托咪酯在神经麻醉中仍然是一种具有吸引人特性的麻醉剂。在灵长类动物模型中,尽管ET剂量极高且脑电图明显受抑制,但神经MEP - SEP仍可重复。此外,在ET爆发抑制性神经保护状态下可监测MEP - SEP。该研究可为人类在基于ET的麻醉下进行术中多模式神经生理记录建立一个模型。

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