首页> 外文期刊>Journal of Neurocytology: A Journal of Cellular Neurobiology >A novel omega-conopeptide for the presynaptic localization of calcium channels at the mammalian neuromuscular junction.
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A novel omega-conopeptide for the presynaptic localization of calcium channels at the mammalian neuromuscular junction.

机译:一种新型的ω-conopepteptide,用于在哺乳动物的神经肌肉连接处进行钙通道的突触前定位。

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摘要

Voltage-sensitive Ca2+ channels are essential to transmitter release at the chemical synapse. To demonstrate the localization of voltage-sensitive Ca2+ channels in relation to the site of transmitter release, mouse neuromuscular junctions were double labelled with alpha-bungarotoxin and a novel voltage-sensitive Ca2+ channel probe, SNX-260, a synthetic analog of omega-conopeptide MVIIC. Similar to omega-conopeptide MVIIC, biotinylated SNX-260 blocked nerve-stimulated transmitter release at the mouse neuromuscular junction. Fluorescently-tagged biotinylated SNX-260 labelled the nerve terminal which appeared thinner than and was outlined by acetylcholine receptor clusters as seen in en face view. This SNX-260 labelling was inhibited by preincubation with unconjugated SNX-260. Side-views of the neuromuscular junction indicated that the SNX-260 labelling was on the synaptic side facing the acetylcholine receptor rather than on the nonsynaptic side of the nerve terminal. This presynaptic binding was confirmed by the absence of SNX-260 labelling in denervated muscles following a nerve cut or disjunction after collagenase treatment. Confocal microscopy revealed spots of SNX-260 labelling that may correlate with active zones. The SNX-260 labelling pattern was not affected by preincubation with unconjugated SNX-111 (omega-conopeptide MVIIA), an N-type voltage-sensitive Ca2+ channel blocker. These findings suggest that SNX-260 is a novel probe for localizing non-N type voltage-sensitive Ca2+ channels and that these voltage-sensitive Ca2+ channels are localized near the transmitter release sites at the mammalian motor nerve terminal membrane. The results are consistent with the suggestion that non-N, probably P/Q type voltage-sensitive Ca2+ channels mediate evoked transmitter release at the mammalian neuromuscular junction.
机译:电压敏感的Ca2 +通道对于化学突触释放变送器至关重要。为了证明电压敏感的Ca2 +通道相对于递质释放部位的定位,小鼠神经肌肉接头用α-真菌毒素和新型的电压敏感的Ca2 +通道探针SNX-260(一种欧米茄泛肽的合成类似物)进行了双重标记。 MVIIC。类似于欧米茄coneptepteptide MVIIC,生物素化的SNX-260在小鼠神经肌肉接头处阻断了神经刺激的递质释放。荧光标记的生物素标记的SNX-260标记了神经末梢,该神经末梢比乙酰胆碱受体簇看起来更细,并在正视时可见。通过与未结合的SNX-260进行预孵育,可以抑制SNX-260标记。神经肌肉接头的侧视图表明,SNX-260标记位于面对乙酰胆碱受体的突触侧,而不是位于神经末梢的非突触侧。胶原酶处理后神经切断或分离后,失神经肌肉中没有SNX-260标记,从而证实了突触前结合。共聚焦显微镜检查发现SNX-260标记斑点可能与活性区域相关。 SNX-260的标记模式不受未偶联的SNX-111(ω-conepteptideMVIIA)(一种N型电压敏感的Ca2 +通道阻滞剂)的预孵育的影响。这些发现表明,SNX-260是用于定位非N型电压敏感Ca2 +通道的新型探针,并且这些电压敏感Ca2 +通道位于哺乳动物运动神经末梢膜的递质释放位点附近。结果与以下观点相符:非N,可能是P / Q型电压敏感的Ca2 +通道介导哺乳动物神经肌肉接头处诱发的递质释放。

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