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A型肉毒杆菌神经毒素对猫展神经运动神经元中gephyrin表达的影响。

Effects of botulinum neurotoxin type A on the expression of gephyrin in cat abducens motoneurons.

作者信息

Moreno-López B, de la Cruz R R, Pastor A M, Delgado-García J M, Alvarez F J

机构信息

Department of Anatomy, Wright State University, Dayton, Ohio, 45435, USA.

出版信息

J Comp Neurol. 1998 Oct 12;400(1):1-17.

PMID:9762863
Abstract

In this study, we investigated the effects of long-term synaptic blockade on postsynaptic receptor clustering at central inhibitory glycinergic synapses. High doses of botulinum neurotoxin type A injected in the lateral rectus muscle completely abolishes inhibitory postsynaptic potentials onto abducens motoneurons within 2 days postinjection, and transmission remains blocked for at least 2 months. Using this model, we analyzed the expression of gephyrin, a glycine receptor clustering protein, on the membrane of motoneuron somata after botulinum neurotoxin type A injection in their target muscle. Immunofluorescence or electron microscopy immunohistochemistry revealed gephyrin-immunoreactive clusters (most < 0.5 microm in diameter) densely covering the surface of control abducens motoneurons. Ultrastructurally, presynaptic terminals containing flattened synaptic vesicles (F terminals) were found associated with multiple gephyrin-immunoreactive postsynaptic densities (average 1.24 gephyrin clusters/F+ profile). No significant changes in gephyrin-immunoreactive clusters were observed at 5 days postinjection, but we found significant reductions (25-40%) in the density of gephyrin clusters 19 and 35 days postinjection. Hence, the physiological alterations reported in this model precede structural changes on postsynaptic receptor cluster density. The decrease in gephyrin-immunoreactive clusters was paralleled by reductions in synaptic covering (F+ terminals per 100 microm of membrane). Presumed inactive F+ terminals that remained attached to the motoneuron surface displayed normal gephyrin-immunoreactive clusters; however, the pre- and postsynaptic membranes in between synaptic active zones frequently appeared separated by enlarged extracellular spaces. We concluded that postsynaptic receptor cluster dissolution seemed more directly related to terminal retraction than to inactivity alone.

摘要

在本研究中,我们调查了长期突触阻断对中枢抑制性甘氨酸能突触后受体聚集的影响。向外侧直肌注射高剂量的A型肉毒杆菌神经毒素,在注射后2天内可完全消除对外展运动神经元的抑制性突触后电位,并且传递至少在2个月内保持阻断状态。利用该模型,我们分析了在其靶肌肉注射A型肉毒杆菌神经毒素后,运动神经元胞体膜上甘氨酸受体聚集蛋白桥连蛋白的表达情况。免疫荧光或电子显微镜免疫组织化学显示,桥连蛋白免疫反应性簇(大多数直径<0.5微米)密集覆盖对照外展运动神经元的表面。在超微结构上,发现含有扁平突触小泡的突触前终末(F终末)与多个桥连蛋白免疫反应性突触后致密物相关(平均1.24个桥连蛋白簇/F+轮廓)。注射后5天未观察到桥连蛋白免疫反应性簇有明显变化,但我们发现在注射后19天和35天桥连蛋白簇的密度显著降低(25-40%)。因此,该模型中报道的生理改变先于突触后受体簇密度的结构变化。桥连蛋白免疫反应性簇的减少与突触覆盖的减少(每100微米膜上的F+终末)平行。仍然附着在运动神经元表面的假定无活性F+终末显示出正常的桥连蛋白免疫反应性簇;然而,突触活跃区之间的突触前和突触后膜经常出现被扩大的细胞外间隙隔开的情况。我们得出结论,突触后受体簇的溶解似乎与终末回缩的关系比单独与无活性的关系更直接。

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