首页> 外文期刊>Frontiers in Physiology >Neurally Released GABA Acts via GABA C Receptors to Modulate Ca 2+ Transients Evoked by Trains of Synaptic Inputs, but Not Responses Evoked by Single Stimuli, in Myenteric Neurons of Mouse Ileum
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Neurally Released GABA Acts via GABA C Receptors to Modulate Ca 2+ Transients Evoked by Trains of Synaptic Inputs, but Not Responses Evoked by Single Stimuli, in Myenteric Neurons of Mouse Ileum

机译:通过GABA C 受体向神经释放的GABA起作用,调节小鼠回肠肌层神经元中由突触输入序列引起的Ca 2 + 瞬变,但不由单一刺激引起。

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γ-Aminobutyric Acid (GABA) and its receptors, GABA_(A,B,C), are expressed in several locations along the gastrointestinal tract. Nevertheless, a role for GABA in enteric synaptic transmission remains elusive. In this study, we characterized the expression and function of GABA in the myenteric plexus of the mouse ileum. About 8% of all myenteric neurons were found to be GABA-immunoreactive (GABA+) including some Calretinin+ and some neuronal nitric oxide synthase (nNOS+) neurons. We used Wnt1-Cre;R26R-GCaMP3 mice, which express a genetically encoded fluorescent calcium indicator in all enteric neurons and glia. Exogenous GABA increased the intracellular calcium concentration, [Ca~(2+)]_(i)of some myenteric neurons including many that did not express GABA or nNOS (the majority), some GABA+, Calretinin+ or Neurofilament-M (NFM)+ but rarely nNOS+ neurons. GABA+ terminals contacted a significantly larger proportion of the cell body surface area of Calretinin+ neurons than of nNOS+ neurons. Numbers of neurons with GABA-induced [Ca~(2+)]_(i)transients were reduced by GABA_(A,B,C)and nicotinic receptor blockade. Electrical stimulation of interganglionic fiber tracts was used to examine possible effects of endogenous GABA release. [Ca~(2+)]_(i)transients evoked by single pulses were unaffected by specific antagonists for each of the 3 GABA receptor subtypes. [Ca~(2+)]_(i)transients evoked by 20 pulse trains were significantly amplified by GABA_(C)receptor blockade. These data suggest that GABA_(A)and GABA_(B)receptors are not involved in synaptic transmission, but suggest a novel role for GABA_(C)receptors in modulating slow synaptic transmission, as indicated by changes in [Ca~(2+)]_(i)transients, within the ENS.
机译:γ-氨基丁酸(GABA)及其受体GABA_(A,B,C)在胃肠道的多个位置表达。尽管如此,GABA在肠道突触传递中的作用仍然难以捉摸。在这项研究中,我们表征了GABA在小鼠回肠肌层神经丛中的表达和功能。发现所有肌层神经元中约有8%是GABA免疫反应性(GABA +),包括一些Calretinin +和一些神经元一氧化氮合酶(nNOS +)神经元。我们使用了Wnt1-Cre; R26R-GCaMP3小鼠,该小鼠在所有肠神经元和神经胶质细胞中表达遗传编码的荧光钙指示剂。外源性GABA增加了一些肌间神经元的细胞内钙浓度[Ca〜(2 +)] _(i),包括许多不表达GABA或nNOS的神经元(大多数),一些GABA +,钙调蛋白+或Neurofilament-M(NFM)+但很少有nNOS +神经元。与nNOS +神经元相比,GABA +末端与Calretinin +神经元的细胞体表面积比例明显更大。 GABA_(A,B,C)和烟碱样受体阻滞减少了GABA诱导的[Ca〜(2 +)] _(i)瞬态的神经元数量。神经节间纤维束的电刺激被用来检查内源性GABA释放的可能影响。对于3种GABA受体亚型中的每一种,由单个脉冲诱发的[Ca〜(2 +)] _(i)瞬变不受特定拮抗剂的影响。通过GABA_(C)受体阻滞显着扩增了20个脉冲序列诱发的[Ca〜(2 +)] _(i)瞬变。这些数据表明,GABA_(A)和GABA_(B)受体不参与突触传递,但暗示了GABA_(C)受体在调节慢突触传递中的新作用,如[Ca〜(2+)的变化所示。 ] _(i)在ENS内瞬变。

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