首页> 美国卫生研究院文献>The Journal of Physiology >Interstitial cells of Cajal are functionally innervated by excitatory motor neurones in the murine intestine
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Interstitial cells of Cajal are functionally innervated by excitatory motor neurones in the murine intestine

机译:Cajal的间质细胞在功能上受鼠肠中兴奋性运动神经元的支配

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摘要

Recent studies have demonstrated that intramuscular interstitial cells of Cajal (ICC) are preferential targets for neurotransmission in the stomach. Terminals of enteric motor neurones also form tight, synaptic-like contacts with ICC in the small intestine and colon, but little is known about the role of these cells in neurotransmission. ICC at the deep muscular plexus (ICC-DMP) of the small intestine express neurokinin 1 receptors (NK1R) and internalize these receptors in response to exogenous substance P. We used NK1R internalization as an assay of functional innervation of ICC-DMP in the murine small intestine. Under basal conditions NK1R-like immunoreactivity (NK1R-LI) was mainly observed in ICC-DMP (519 cells counted, 100% were positive) and myenteric neurones. ICC-DMP were closely apposed to substance P-containing nerve fibres. Of 338 ICC-DMP examined, 65% were closely associated with at least one substance P-positive nerve fibre, 32% were associated with at least two, 2% were associated with more than two nerve fibres and 1% with none. After electrical field stimulation (EFS, 10 Hz; 1 min) NK1R-LI was internalized in more than 80% of ICC-DMP, as compared to 10% of cells before EFS. Internalization of NK1R was not observed in myenteric ICC or smooth muscle cells in response to nerve stimulation. Internalization of NK1R-LI was blocked by the specific NK1 receptor antagonist WIN 62577 (1 μm) and by tetrodotoxin (0.3 μm), suggesting that internalization resulted from stimulation of receptors with neurally released neurokinins. These data suggest that ICC-DMP are primary targets for neurokinins released from enteric motor neurones in the intestine.
机译:最近的研究表明,Cajal的肌间质细胞(ICC)是胃中神经传递的优先靶标。肠运动神经元的末端还与小肠和结肠中的ICC形成紧密的突触样接触,但对这些细胞在神经传递中的作用知之甚少。小肠深层神经丛(ICC-DMP)上的ICC表达神经激肽1受体(NK1R)并内化这些受体以响应外源物质P。我们使用NK1R内化作为小鼠中ICC-DMP功能神经支配的测定小肠。在基础条件下,主要在ICC-DMP(计数为519个细胞,100%阳性)和肌层神经元中观察到了NK1R样免疫反应性(NK1R-LI)。 ICC-DMP与含P物质的神经纤维紧密相连。在检查的338例ICC-DMP中,有65%与至少一种P阳性神经纤维紧密相关,有32%与至少两种P阳性神经纤维紧密相关,有2%与多于两条神经纤维相关,有1%与无神经纤维相关。电场刺激(EFS,10 Hz; 1分钟)后,NK1R-LI被内在超过80%的ICC-DMP中,而EFS前为10%的细胞。在肌层ICC或平滑肌细胞中未观察到NK1R对神经刺激的内在化。 NK1R-LI的内部化被特定的NK1受体拮抗剂WIN 62577(1μm)和河豚毒素(0.3μm)阻断,这表明内部化是由于神经释放的神经激肽刺激受体所致。这些数据表明,ICC-DMP是肠内肠道运动神经元释放的神经激肽的主要靶标。

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