首页> 美国卫生研究院文献>The Journal of Physiology >Non-dopaminergic neurones of the reticular part of substantia nigra can gate static fusimotor action onto flexors in cat.
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Non-dopaminergic neurones of the reticular part of substantia nigra can gate static fusimotor action onto flexors in cat.

机译:黑质网状部分的非多巴胺能神经元可以控制猫的屈肌上的静态融合运动。

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摘要

The effect on the fusimotor system of electrical stimulation of the reticular part of the substantia nigra or of the injection of the gamma-aminobutyric acid (GABA)-antagonist picrotoxin into this structure was studied in spindle receptors of pretibial flexors in cats anaesthetized with ketamine. Afferent activity of muscle spindle primary endings was recorded before and during these two forms of intranigral stimulation. Dynamic spindle sensitivity was assessed during both small- (100 microns) and large-amplitude (2 mm) sinusoidal stretching of the receptor-bearing muscles. From changes in spindle sensitivity after nigral electrical stimulation (eleven out of fourteen primary endings) or intranigral injection of picrotoxin (fifty-one out of sixty-seven primary endings) it is deduced that functional activation of neurones of the reticular part of substantia nigra, in this preparation, removed a normally present tonic static fusimotor action from the primary sensory endings of pretibial flexor muscle spindles. This effect, induced by picrotoxin (2 micrograms in 1 microliter), was reversed by a subsequent intranigral injection of the GABA-agonist muscimol (0.4 microgram in 1 microliters), but remained unchanged after subsequent intracaudate injections of haloperidol (12.5 micrograms in 5 microliters) or apomorphine (5 micrograms in 5 microliters). It is concluded that the C.N.S. can gate static fusimotor action onto flexor muscle spindle primary endings through non-dopaminergic output neurones of the reticular part of substantia nigra.
机译:在氯胺酮麻醉的猫的前屈肌纺锤体受体中研究了电刺激黑质网状部分或向该结构中注射γ-氨基丁酸(GABA)-拮抗剂微毒素对融合运动系统的影响。在这两种形式的鼻内刺激之前和期间记录肌肉纺锤初级末梢的传入活动。在带有受体的肌肉的小振幅(100微米)和大振幅(2毫米)正弦曲线拉伸过程中评估了动态纺锤体敏感性。从黑电刺激(十四个初级末端中的十一个)或鼻内注射微毒素(六十七个初级末端中的五十一个)后的主轴敏感性变化,可以推断出黑质网状部分神经元的功能激活,在该制剂中,从胫前屈肌梭的主要感觉末端去除了正常存在的强直静态动作。随后通过鼻内注射GABA激动剂麝香酚(1微升为0.4微克)逆转了由微毒素(1微升中为2微克)诱导的这种作用,但在随后的尾状氟哌啶醇尾巴内注射(5微升中为12.5微克)后,这种作用得以逆转。 )或阿扑吗啡(5微升/ 5微升)。结论是C.N.S.可以通过黑质网状部分的非多巴胺能输出神经元将静态融合运动控制在屈肌主轴的主要末端。

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