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首页> 外文期刊>Autonomic neuroscience: basic & clinical >Differential inhibitory control of circular and longitudinal smooth muscle layers of Balb/C mouse small intestine.
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Differential inhibitory control of circular and longitudinal smooth muscle layers of Balb/C mouse small intestine.

机译:Balb / C小鼠小肠圆形和纵向平滑肌层的差异抑制控制。

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We examined the inhibitory mediators acting on each of the longitudinal (LM) and circular muscle (CM) layers of mouse small intestine in the presence of atropine, prazosin and timolol. Nitric oxide (NO) and apamin-sensitive mediators exerted an inhibitory tone on pacing frequency in CM, observed as an increased frequency upon treatment with N-omega-nitro-l-arginine (LNNA) or apamin. This effect was not seen in LM. 1H-(1,2,4)oxadiazolo(4,3-A)quinazoline-1-one (ODQ) abolished the relaxation in response to electric field stimulation (EFS) in LM in a manner similar to LNNA indicating that the inhibitory mediator in this layer in NO acting via soluble guanylate cyclase. On the other hand, in CM neither LNNA nor apamin was capable of reducing the inhibition in response to EFS and their combination left a residual relaxation of 25%. ODQ reduced the EFS-evoked relaxation more effectively than LNNA at higher frequencies indicating that another ODQ-sensitive mediator was active in CM. ODQ also blocked the relaxation to exogenous vasoactive intestinal peptide in CM. In LM, the relaxation due to sodium nitroprusside was equally blocked by ODQ and apamin, while in CM, its effects were only reduced by ODQ and not apamin. These results indicate that there are differences in the inhibitory mediators and the mechanisms of action involved in LM and CM relaxation.
机译:我们检查了在存在阿托品,哌唑嗪和噻吗洛尔的情况下,对小鼠小肠的纵向(LM)和环形肌肉(CM)层的抑制介质的作用。一氧化氮(NO)和对apapamin敏感的介体对CM的起搏频率起抑制作用,观察到用N-ω-硝基-1-精氨酸(LNNA)或apaapamin处理时频率增加。在LM中看不到这种效果。 1H-(1,2,4)恶二唑(4,3-A)喹唑啉-1-一(ODQ)消除了LM中响应电场刺激(EFS)的松弛,其方式类似于LNNA,表明该抑制介质在该层中,NO通过可溶性鸟苷酸环化酶起作用。另一方面,在CM中,LNNA和apaapamin均不能降低对EFS的抑制作用,并且它们的组合留下了25%的残留松弛。在较高频率下,ODQ比LNNA更有效地降低了EFS引起的舒张,表明另一种ODQ敏感介体在CM中活跃。 ODQ还阻止了CM中外源血管活性肠肽的松弛。在LM中,由硝普钠引起的松弛被ODQ和阿帕明同等地阻断,而在CM中,其作用仅被ODQ而不是阿帕明减弱。这些结果表明,LM和CM松弛所涉及的抑制介质和作用机理存在差异。

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