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全身麻醉药对猫脊髓Ia类兴奋性突触后电位和电流的抑制作用。

Reduction by general anaesthetics of group Ia excitatory postsynaptic potentials and currents in the cat spinal cord.

作者信息

Kullmann D M, Martin R L, Redman S J

机构信息

Experimental Neurology Unit, John Curtin School of Medical Research, Canberra, ACT, Australia.

出版信息

J Physiol. 1989 May;412:277-96. doi: 10.1113/jphysiol.1989.sp017615.

Abstract
  1. The effects of thiopentone and halothane on excitatory synaptic transmission at group Ia afferent synapses on lumbosacral motoneurones were studied in the anaesthetized or decerebrate cat. 2. Thiopentone (10 mg kg-1) infused on a background of light pentobarbitone anaesthesia caused a decrease in single-fibre monosynaptic group Ia excitatory postsynaptic potentials (EPSPs) of between 0 and 24%. A step increase in inspired halothane concentration in the range 0.7-0.9% produced a decrease in EPSP amplitude of between 0 and 31%. These effects were reversible when the anaesthetic level was reduced. 3. Fluctuation analysis of selected single-fibre group Ia EPSPs revealed that these effects could be accounted for by a decrease in the probability of occurrence of EPSPs of larger amplitude, and an increase in the probability of occurrence of EPSPs of smaller amplitude. The mean separation between discrete amplitudes was not altered by either anaesthetic agent. 4. EPSPs whose time course indicated a somatic site of origin were voltage clamped to study the effect of the anaesthetics on the time course of the synaptic currents. Neither thiopentone nor halothane produced a consistent effect on the time constant of decay of the current, although they both depressed its peak amplitude. 5. The results are interpreted as indicating a presynaptic site of action of both anaesthetics at the concentrations studied: the probability of release of neurotransmitter is reduced, without any detectable change in the mean duration of the postsynaptic conductance increase. These findings are discussed in relation to the mechanisms of action of anaesthetics on exocytosis and presynaptic inhibition.
摘要
  1. 在麻醉或去大脑的猫身上,研究了硫喷妥钠和氟烷对腰荐运动神经元Ia类传入突触兴奋性突触传递的影响。2. 在轻度戊巴比妥麻醉背景下输注硫喷妥钠(10毫克/千克),导致单纤维单突触Ia类兴奋性突触后电位(EPSP)降低0%至24%。将吸入的氟烷浓度逐步提高到0.7 - 0.9%,会使EPSP幅度降低0%至31%。当麻醉水平降低时,这些效应是可逆的。3. 对选定的单纤维Ia类EPSP进行波动分析表明,这些效应可以通过较大幅度EPSP出现概率的降低和较小幅度EPSP出现概率的增加来解释。两种麻醉剂均未改变离散幅度之间的平均间距。4. 对时间进程表明起源于躯体部位的EPSP进行电压钳制,以研究麻醉剂对突触电流时间进程的影响。硫喷妥钠和氟烷均未对电流衰减的时间常数产生一致的影响,尽管它们都降低了电流的峰值幅度。5. 结果被解释为表明在所研究的浓度下,两种麻醉剂的作用位点均在突触前:神经递质释放的概率降低,而突触后电导增加的平均持续时间没有任何可检测到的变化。结合麻醉剂对胞吐作用和突触前抑制的作用机制对这些发现进行了讨论。

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