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Changes in binomial parameters of quantal release at crustacean motor axon terminals during presynaptic inhibition.

机译:突触前抑制过程中甲壳动物运动轴突末端定量释放的二项式参数的变化。

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摘要

1. The effects of presynaptic inhibition on quantal release of transmitter were investigated at neuromuscular junctions of the motor axon supplying one of the limb muscles of a crab (Pachygrapsus crassipes). 2. Binomial analysis of transmitter release recorded at selected neuromuscular junctions with an extracellular 'macro-patch' electrode indicated high probability of release (p) from a limited number of available sites (n). During presynaptic inhibition, both n and p were reduced. 3. The binomial model provided a good description of results from non-inhibited junctions. During presynaptic inhibition, results from some junctions could be described by the binomial model, while those from other junctions could not. An interpretation of this finding is that presynaptic inhibition differentially affects the probability of release at various release sites of the neuromuscular junctional complex. 4. A morphological study of the region of transmitter release under the macropatch electrode was made. Release-dependent uptake of horseradish peroxidase (HRP) into presynaptic terminals was restricted to the region under the recording electrode, by perfusing the preparation with calcium-free solution containing HRP. Transmitter release, and HRP uptake, occurred only at the site of the electrode, which was filled with a calcium-containing solution. Subsequently, serial sections were prepared for electron microscopy and the region of transmitter release was reconstructed. 5. Numerous axo-axonal synapses were found in the HRP-labelled region. Thus, the morphological prerequisite for presynaptic inhibition exists at the site of transmitter release, and not exclusively at a more remote region. 6. The number of morphologically identified excitatory neuromuscular synapses exceeded the 'release sites' estimated from the binomial model (n) by a wide margin. Morphological differences among synapses were observed. It is proposed that not all morphologically identified synapses participated in transmitter release under the experimental conditions employed. Thus, morphologically defined synapses are likely to be non-uniform in their response properties, including probability of transmitter release (p).
机译:1.在供应蟹的四肢肌肉之一的运动轴突的神经肌肉接头处,研究了突触前抑制对递质定量释放的影响。 2.用细胞外“宏贴”电极在选定的神经肌肉接头处记录的递质释放的二项式分析表明,从有限数量的可用位点(n)释放的可能性很高(p)。在突触前抑制过程中,n和p均降低。 3.二项式模型很好地描述了非抑制连接的结果。在突触前抑制期间,可以通过二项式模型描述某些连接的结果,而其他连接的结果则无法。该发现的解释是,突触前抑制差异性地影响神经肌肉接头复合体各个释放部位的释放概率。 4.对大面膜电极下的递质释放区域进行了形态学研究。通过用含HRP的无钙溶液灌注制剂,将与释放有关的辣根过氧化物酶(HRP)摄取到突触前末端限制在记录电极下方的区域。变送器释放和HRP吸收仅发生在电极的位置,该位置充满了含钙溶液。随后,准备了用于电子显微镜的连续切片,并重建了发射器释放区域。 5.在HRP标记的区域发现了许多轴突-轴突突触。因此,突触前抑制的形态学先决条件存在于递质释放的位点,而不仅仅是在较远的区域。 6.形态学上确定的兴奋性神经肌肉突触的数量大大超出了从二项式模型(n)估计的“释放部位”。观察到突触之间的形态学差异。建议在所采用的实验条件下,并非所有形态学鉴定的突触均参与递质的释放。因此,形态学定义的突触的响应特性(包括发射器释放的概率)可能很不均匀。

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