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首页> 外文期刊>American Journal of Physiology >Subtypes of muscarinic receptors regulating gallbladder cholinergic contractions.
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Subtypes of muscarinic receptors regulating gallbladder cholinergic contractions.

机译:调节胆囊胆碱能收缩的毒蕈碱受体的亚型。

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The aim of this study was to determine the functional role of muscarinic receptor subtypes regulating gallbladder cholinergic contractions. Electrical field stimulation (EFS; 16 Hz) produced contractile responses of guinea pig gallbladder muscle strips in vitro that were inhibited by 1 microM tetrodotoxin (2 +/- 2% of control) and 1 microM atropine (1 +/- 1% of control), indicating activation of intrinsic cholinergic nerves. Exogenous ACh (5 microM)-induced contractions were inhibited by atropine (1 +/- 1% of control) but not tetrodotoxin (102 +/- 1% of control), indicating a direct effect on smooth muscle. The M1 receptor antagonist pirenzepine (10 nM) had no effect on ACh-induced contractions but inhibited EFS-induced contractions by 11 +/- 3%. The M2 antagonist methoctramine (10 nM) had no effect on ACh-induced contractions but augmented EFS-induced contractions by 5 +/- 2%. The M3 antagonist 4-DAMP (10 nM) inhibited ACh-induced contractions by 14 +/- 4% and EFS-induced contractions by 22 +/- 5%. In conclusion, specific M1, M2, and M3 receptors modulate gallbladder muscle contractions by regulating ACh release from cholinergic nerves and mediating the contraction. Cholinergic contractions are mediated by M3 receptors directly on the smooth muscle. M2 receptors are on cholinergic nerves and function as prejunctional inhibitory autoreceptors. M1 receptors are on cholinergic nerves and function as prejunctional facilitatory autoreceptors.
机译:这项研究的目的是确定调节胆囊胆碱能收缩的毒蕈碱受体亚型的功能作用。电场刺激(EFS; 16 Hz)在体外产生豚鼠胆囊肌条的收缩反应,被1 microM河豚毒素(对照组的2 +/- 2%)和1 microM阿托品(对照组的1 +/- 1%)抑制),表明内在胆碱能神经被激活。阿托品(对照的1 +/- 1%)抑制了外源性ACh(5 microM)引起的收缩,但河豚毒素(对照的102 +/- 1%)则抑制了收缩,表明对平滑肌有直接作用。 M1受体拮抗剂哌仑西平(10 nM)对ACh诱导的收缩无影响,但抑制EFS诱导的收缩11 +/- 3%。 M2拮抗剂甲基辛特拉明(10 nM)对ACh诱导的收缩无影响,但使EFS诱导的收缩增加5 +/- 2%。 M3拮抗剂4-DAMP(10 nM)抑制ACh诱导的收缩14 +/- 4%,抑制EFS诱导的收缩22 +/- 5%。总之,特定的M1,M2和M3受体通过调节胆碱能神经释放ACh并介导收缩来调节胆囊肌肉收缩。胆碱能收缩直接由平滑肌上的M3受体介导。 M2受体位于胆碱能神经上,起结前抑制性自体受体的作用。 M1受体位于胆碱能神经上,起结前促进性自体受体的作用。

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