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大鼠海马体单一突触处的双脉冲易化和抑制:量子涨落影响后续释放。

Paired-pulse facilitation and depression at unitary synapses in rat hippocampus: quantal fluctuation affects subsequent release.

作者信息

Debanne D, Guérineau N C, Gähwiler B H, Thompson S M

机构信息

Brain Research Institute, University of Zurich, Switzerland.

出版信息

J Physiol. 1996 Feb 15;491 ( Pt 1)(Pt 1):163-76. doi: 10.1113/jphysiol.1996.sp021204.

Abstract
  1. Excitatory synaptic transmission between pairs of monosynaptically coupled pyramidal cells was examined in rat hippocampal slice cultures. Action potentials were elicited in single CA3 pyramidal cells impaled with microelectrodes and unitary excitatory postsynaptic currents (EPSCs) were recorded in whole-cell voltage-clamped CA1 or CA3 cells. 2. The amplitude of successive unitary EPSCs in response to single action potentials varied. The amplitude of EPSCs was altered by adenosine or changes in the [Mg2+]/[CA2+] ratio. We conclude that single action potentials triggered the release of multiple quanta of glutamate. 3. When two action potentials were elicited in the presynaptic cell, the amplitude of the second EPSC was inversely related to the amplitude of the first. Paired-pulse facilitation (PPF) was observed when the first EPSC was small, i.e. the second EPSC was larger than the first, whereas paired-pulse depression (PPD) was observed when the first EPSC was large. 4. The number of trials displaying PPD was greater when release probability was increased, and smaller when release probability was decreased. 5. PPD was not postsynaptically mediated because it was unaffected by decreasing ionic flux with 6-cyano-7-nitroquinoxaline-2,3-dione (CNQX) or receptor desensitization with aniracetam. 6. PPF was maximal at an interstimulus interval of 70 ms and recovered within 500 ms. Recovery from PPD occurred within 5 s. 7. We propose that multiple release sites are formed by the axon of a CA3 pyramidal cell and a single postsynaptic CA1 or CA3 cell. PPF is observed if the first action potential fails to release transmitter at most release sites. PPD is observed if the first action potential successfully triggers release at most release sites. 8. Our observations of PPF are consistent with the residual calcium hypothesis. We conclude that PPD results from a decrease in quantal content, perhaps due to short-term depletion of readily releasable vesicles.
摘要
  1. 在大鼠海马切片培养物中检测了成对单突触耦合锥体细胞之间的兴奋性突触传递。用微电极刺入单个CA3锥体细胞诱发动作电位,并在全细胞电压钳制的CA1或CA3细胞中记录单位兴奋性突触后电流(EPSC)。2. 响应单个动作电位的连续单位EPSC的幅度各不相同。腺苷或[Mg2+]/[Ca2+]比值的变化会改变EPSC的幅度。我们得出结论,单个动作电位触发了多个谷氨酸量子的释放。3. 当在突触前细胞中诱发两个动作电位时,第二个EPSC的幅度与第一个呈负相关。当第一个EPSC较小时观察到双脉冲易化(PPF),即第二个EPSC大于第一个,而当第一个EPSC较大时观察到双脉冲抑制(PPD)。4. 当释放概率增加时,显示PPD的试验次数更多,而当释放概率降低时则更少。5. PPD不是由突触后介导的,因为它不受用6-氰基-7-硝基喹喔啉-2,3-二酮(CNQX)降低离子通量或用茴拉西坦使受体脱敏的影响。6. PPF在70毫秒的刺激间隔时最大,并在500毫秒内恢复。从PPD恢复发生在5秒内。7. 我们提出,多个释放位点由CA3锥体细胞的轴突与单个突触后CA1或CA3细胞形成。如果第一个动作电位在大多数释放位点未能释放递质,则观察到PPF。如果第一个动作电位在大多数释放位点成功触发释放,则观察到PPD。8. 我们对PPF的观察结果与残余钙假说一致。我们得出结论,PPD是由于量子含量减少所致, 可能是由于易释放囊泡的短期耗竭。

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