Integrated responses of the SIP syncytium generate a major motility pattern in the colon

IF 4.7 2区医学 Q1 NEUROSCIENCES Journal of Physiology-London Pub Date : 2024-11-21 DOI:10.1113/JP287315

Sang Don Koh, Ji Yeon Lee, Seung-Bum Ryoo, Bernard T. Drumm, Hyun Jin Kim, Sal A. Baker, Kenton M. Sanders

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Abstract

The peristaltic reflex has been a central concept in gastrointestinal motility; however, evidence was published recently suggesting that post-stimulus responses that follow inhibitory neural responses provide the main propulsive force in colonic motility. This new concept was based on experiments on proximal colon where enteric inhibitory neural inputs are mainly nitrergic. However, the nature of inhibitory neural inputs changes from proximal to distal colon where purinergic inhibitory regulation dominates. In spite of the transition from nitrergic to purinergic regulation, post-stimulus responses and propulsive contractions were both blocked by antagonists of a conductance (ANO1) exclusive to interstitial cells of Cajal (ICC). How purinergic neurotransmission, transduced by PDGFRα⁺ cells, can influence ANO1 in ICC is unknown. We compared neural responses in proximal and distal colon. Post-stimulus responses were blocked by inhibition of nitrergic neurotransmission in proximal colon, but P2Y1 receptor antagonists were more effective in distal colon. Ca²⁺ entry through voltage-dependent channels (Ca_V3) enhances Ca²⁺ release in ICC. Thus, we reasoned that hyperpolarization caused by purinergic responses in PDGFRα⁺ cells, which are electrically coupled to ICC, might decrease inactivation of Ca_V3 channels and activate Ca²⁺ entry into ICC via anode-break upon cessation of inhibitory responses. Post-stimulus responses in distal colon were blocked by MRS2500 (P2Y1 receptor antagonist), apamin (SK channel antagonist) and NNC55-0396 (Ca_V3 antagonist). These compounds also blocked propagating contractions in mid and distal colon. These data provide the first clear demonstration that integration of functions in the smooth muscle–ICC–PDGFRα⁺ cell (SIP) syncytium generates a major motility behaviour.

Key points

Propagating propulsive contractions initiated by the enteric nervous system are a major motility behaviour in the colon. A major component of contractions, necessary for propulsive contractions, occurs at cessation of enteric inhibitory neurotransmission (post-stimulus response) and is generated by interstitial cells of Cajal (ICC), which are electrically coupled to smooth muscle cells.
The nature of enteric inhibitory neurotransmission shifts from proximal colon, where it is predominantly due to nitric oxide, to distal colon, where it is predominantly due to purine neurotransmitters.
Different cells transduce nitric oxide and purines in the colon. ICC transduce nitric oxide, but another type of interstitial cell, PDGFRα⁺ cells, transduces input from purinergic neurons.
However, the post-stimulus responses in proximal and distal colon are still generated in ICC.
This paper explores how integrated behaviours of ICC, PDGFRα⁺ cells and smooth muscle cells accomplish propulsive motility in the colon.

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SIP 合胞体的综合反应产生了结肠的主要运动模式。

蠕动反射一直是胃肠道运动的核心概念；然而，最近发表的证据表明，抑制性神经反应之后的刺激后反应是结肠运动的主要推动力。这一新概念基于近端结肠的实验，在近端结肠中，肠抑制性神经输入主要是硝酸神经输入。然而，从近端结肠到远端结肠，抑制性神经输入的性质发生了变化，在远端结肠中，嘌呤能抑制调节占主导地位。尽管从硝酸能调节过渡到了嘌呤能调节，但刺激后反应和推进性收缩均被卡贾尔间质细胞（ICC）特有的传导（ANO1）拮抗剂阻断。由 PDGFRα+ 细胞转导的嘌呤能神经传递如何影响 ICC 中的 ANO1 尚不清楚。我们比较了近端和远端结肠的神经反应。抑制近端结肠的硝酸神经递质可阻断刺激后反应，但 P2Y1 受体拮抗剂对远端结肠更有效。通过电压依赖性通道（CaV3）进入的 Ca2+ 会增强 ICC 中 Ca2+ 的释放。因此，我们推断，与 ICC 电耦合的 PDGFRα+ 细胞中嘌呤能反应引起的超极化可能会降低 CaV3 通道的失活，并在抑制性反应停止后通过阳极断裂激活 Ca2+ 进入 ICC。MRS2500（P2Y1 受体拮抗剂）、阿帕明（SK 通道拮抗剂）和 NNC55-0396（CaV3 拮抗剂）可阻断远端结肠的刺激后反应。这些化合物也阻断了中段和远段结肠的传播性收缩。这些数据首次明确证明，平滑肌-ICC-表皮生长因子受体α+细胞（SIP）合胞的功能整合会产生主要的运动行为。要点由肠道神经系统引发的推进性收缩是结肠的一种主要运动行为。推动性收缩所必需的收缩的一个主要部分发生在肠抑制性神经传递停止时（刺激后反应），由与平滑肌细胞电耦合的卡亚尔间质细胞（ICC）产生。肠道抑制性神经传递的性质从结肠近端转移到结肠远端，在结肠近端主要是一氧化氮，而在结肠远端主要是嘌呤神经递质。结肠中转导一氧化氮和嘌呤的细胞不同。ICC 转导一氧化氮，但另一类间质细胞 PDGFRα+ 细胞则转导来自嘌呤能神经元的输入。然而，近端和远端结肠的刺激后反应仍由 ICC 产生。本文探讨了 ICC、PDGFRα+ 细胞和平滑肌细胞的综合行为如何完成结肠的推进运动。

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来源期刊

Journal of Physiology-London 医学-神经科学

CiteScore

9.70

自引率

7.30%

发文量

817

审稿时长

2 months

期刊介绍： The Journal of Physiology publishes full-length original Research Papers and Techniques for Physiology, which are short papers aimed at disseminating new techniques for physiological research. Articles solicited by the Editorial Board include Perspectives, Symposium Reports and Topical Reviews, which highlight areas of special physiological interest. CrossTalk articles are short editorial-style invited articles framing a debate between experts in the field on controversial topics. Letters to the Editor and Journal Club articles are also published. All categories of papers are subjected to peer reivew. The Journal of Physiology welcomes submitted research papers in all areas of physiology. Authors should present original work that illustrates new physiological principles or mechanisms. Papers on work at the molecular level, at the level of the cell membrane, single cells, tissues or organs and on systems physiology are all acceptable. Theoretical papers and papers that use computational models to further our understanding of physiological processes will be considered if based on experimentally derived data and if the hypothesis advanced is directly amenable to experimental testing. While emphasis is on human and mammalian physiology, work on lower vertebrate or invertebrate preparations may be suitable if it furthers the understanding of the functioning of other organisms including mammals.