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健康大鼠膀胱中功能性毒蕈碱敏感的嘌呤能反应。

Functional atropine sensitive purinergic responses in the healthy rat bladder.

机构信息

Department of Pharmacology, Institute of Neuroscience and Physiology, Sahlgrenska Academy at the University of Gothenburg, Box 431, 405 30 Gothenburg, Sweden.

出版信息

Auton Neurosci. 2020 Sep;227:102693. doi: 10.1016/j.autneu.2020.102693. Epub 2020 Jun 9.

DOI:10.1016/j.autneu.2020.102693
PMID:32563054
Abstract

While acetylcholine is regarded to be the main directly contractile transmitter substance in the urinary bladder, interactions with other transmitters likely occur. Presently, the interplay between purinergic and cholinergic signalling was investigated to unravel the involvement of the urothelium and efferent neurons in the functionally important purinergically evoked release of acetylcholine in vitro. Functional characterization of receptor subtypes involved in this interplay was also performed. In vitro organ bath experiments with electrical field stimulation (EFS) or administration of agonist were performed in the absence and presence of the neurotoxin tetrodotoxin (TTX; 5 × 10 M) and/or receptor antagonists, in intact and urothelium-denuded full thickness rat bladder strip preparations. Interestingly, functional contractions to ATP (10-10 M) remained unaffected by TTX, but were significantly lowered in the presence of the muscarinic antagonist atropine (10 M). However, in urothelium-denuded strip preparations, this latter phenomenon was not present and the ATP response remained unaltered. To rule out purinergic interference caused by break-down of ATP, experiments were performed in which the stable ATP-analogue αβMeATP (10-10 M) gave rise to functional atropine-sensitive contractions. Furthermore, contractions to ATP were not affected by P2Y6 purinoceptor blockade (by MRS2578; 10, 10 M), nor were relaxatory responses to ATP sensitive to atropine, PPADS (3 × 10 M) or αβMeATP. Lastly, relaxations to ADP (10-10 M) or NECA (10-10 M) were unaltered by the presence of atropine. To conclude, purinergic functional contractile, but not relaxatory, responses are supported by the cholinergic transmitter system in vitro, through non-neuronal mechanisms in the urothelium. Involved purinoceptors are of the P2X-subtype, most likely P2X1 and/or P2X3.

摘要

虽然乙酰胆碱被认为是膀胱中主要的直接收缩性递质物质,但它与其他递质之间可能存在相互作用。目前,研究了嘌呤能和胆碱能信号之间的相互作用,以揭示在上皮细胞和传出神经元在体外功能重要的嘌呤能诱发乙酰胆碱释放中的作用。还对参与这种相互作用的受体亚型进行了功能特征分析。在不存在和存在神经毒素河豚毒素 (TTX; 5×10-6 M) 和/或受体拮抗剂的情况下,在完整和去上皮的全层大鼠膀胱条带制备物中,进行了电刺激 (EFS) 或激动剂给药的离体器官浴实验。有趣的是,ATP (10-10 M) 的功能收缩不受 TTX 影响,但在存在毒蕈碱拮抗剂阿托品 (10-6 M) 的情况下明显降低。然而,在上皮细胞去极化的条带制备物中,这种现象不存在,并且 ATP 反应保持不变。为了排除由于 ATP 分解引起的嘌呤能干扰,进行了实验,其中稳定的 ATP 类似物 αβMeATP (10-10 M) 引起功能上的阿托品敏感收缩。此外,ATP 引起的收缩不受 P2Y6 嘌呤能受体阻断剂 (MRS2578; 10, 10-6 M) 的影响,对 ATP 的弛豫反应也不受阿托品、PPADS (3×10-6 M) 或 αβMeATP 的影响。最后,ADP (10-10 M) 或 NECA (10-10 M) 引起的弛豫不受阿托品的影响。总之,嘌呤能功能性收缩,但不是弛豫反应,是通过上皮细胞中的非神经元机制,在体外由胆碱能递质系统支持的。涉及的嘌呤能受体是 P2X 亚基型,很可能是 P2X1 和/或 P2X3。

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