在去大脑犬模型中，七氟醚增强A型γ-氨基丁酸受体功能并全面抑制吸气前运动神经元。

Sevoflurane enhances gamma-aminobutyric acid type A receptor function and overall inhibition of inspiratory premotor neurons in a decerebrate dog model.

作者信息

Stucke Astrid G, Zuperku Edward J, Krolo Mirko, Brandes Ivo F, Hopp Francis A, Kampine John P, Stuth Eckehard A E

机构信息

Department of Anesthesiology, Medical College of Wisconsin, Milwaukee, USA.

出版信息

Anesthesiology. 2005 Jul;103(1):57-64. doi: 10.1097/00000542-200507000-00012.

DOI:10.1097/00000542-200507000-00012

PMID:15983457

Abstract

BACKGROUND

Inspiratory premotor neurons in the caudal ventral medulla relay excitatory drive to phrenic and inspiratory intercostal motoneurons in the spinal cord. These neurons are subject to tonic gamma-aminobutyric acid type A (GABAA)ergic inhibition. In a previous study, 1 minimum alveolar concentration (MAC) sevoflurane depressed overall glutamatergic excitatory drive and enhanced overall GABAAergic inhibitory drive to the neurons. This study investigated in further detail the effects of sevoflurane on GABAAergic inhibition by examining postsynaptic GABAA receptor activity in these neurons.

METHODS

Studies were performed in decerebrate, vagotomized, paralyzed, and mechanically ventilated dogs during hypercapnic hyperoxia. The effect of 1 MAC sevoflurane on extracellularly recorded neuronal activity was measured during localized picoejection of the GABAA receptor antagonist bicuculline and the GABAA agonist muscimol. Complete blockade of GABAAergic inhibition by bicuculline allowed estimation of the prevailing overall inhibition of the neuron. The neuronal response to muscimol was used to assess the anesthetic effect on the postsynaptic GABAA receptor function.

RESULTS

One MAC sevoflurane depressed the spontaneous activity of 21 inspiratory premotor neurons by (mean +/- SD) 32.6 +/- 20.5% (P < 0.001). Overall excitatory drive was depressed 17.9 +/- 19.8% (P < 0.01). Overall GABAAergic inhibition was enhanced by 18.5 +/- 18.2% (P < 0.001), and the postsynaptic GABAA receptor function was increased by 184.4 +/- 121.8% (n = 20; P < 0.001).

CONCLUSION

One MAC sevoflurane greatly enhanced GABAA receptor function on inspiratory premotor neurons and increased overall synaptic inhibition but to a smaller extent, indicating that the presynaptic inhibitory input was also reduced. Therefore, the anesthetic depression of spontaneous inspiratory premotor neuronal activity by 1 MAC sevoflurane in vivo is due to a combined effect on the two major ionotropic synaptic neurotransmitter systems with a decrease in overall glutamatergic excitation and a strong enhancement of postsynaptic GABAA receptor function.

摘要

背景

延髓尾端腹侧的吸气前运动神经元将兴奋性冲动传递至脊髓中的膈神经运动神经元和吸气性肋间运动神经元。这些神经元受到持续性γ-氨基丁酸A型（GABAA）能抑制作用的影响。在之前的一项研究中，1个最低肺泡有效浓度（MAC）的七氟醚可抑制这些神经元的整体谷氨酸能兴奋性冲动，并增强整体GABAA能抑制性冲动。本研究通过检测这些神经元的突触后GABAA受体活性，进一步详细探究七氟醚对GABAA能抑制作用的影响。

方法

在高碳酸血症性高氧状态下，对去大脑、切断迷走神经、麻痹并机械通气的犬进行研究。在局部微量注射GABAA受体拮抗剂荷包牡丹碱和GABAA激动剂蝇蕈醇期间，测量1个MAC七氟醚对细胞外记录的神经元活动的影响。荷包牡丹碱对GABAA能抑制作用的完全阻断使得能够估计神经元当前的整体抑制情况。神经元对蝇蕈醇的反应用于评估麻醉药对突触后GABAA受体功能的影响。

结果

1个MAC七氟醚使21个吸气前运动神经元的自发活动降低了（均值±标准差）32.6±20.5%（P<0.001）。整体兴奋性冲动降低了17.9±19.8%（P<0.01）。整体GABAA能抑制作用增强了18.5±18.2%（P<0.001），突触后GABAA受体功能增加了184.4±121.8%（n = 20；P<0.001）。

结论

1个MAC七氟醚极大地增强了吸气前运动神经元上的GABAA受体功能，并增加了整体突触抑制，但程度较小，表明突触前抑制性输入也减少了。因此，在体内，1个MAC七氟醚对吸气前运动神经元自发活动的麻醉性抑制作用是由于对两个主要的离子型突触神经递质系统的联合作用，即整体谷氨酸能兴奋性降低以及突触后GABAA受体功能的强烈增强。