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首页> 外文期刊>Neuroscience Letters: An International Multidisciplinary Journal Devoted to the Rapid Publication of Basic Research in the Brain Sciences >Synergism between A(2A)-adenosine receptor activation and vasoactive intestinal peptide to facilitate (3H)-acetylcholine release from the rat motor nerve terminals.
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Synergism between A(2A)-adenosine receptor activation and vasoactive intestinal peptide to facilitate (3H)-acetylcholine release from the rat motor nerve terminals.

机译:A(2A)-腺苷受体激活和血管活性肠肽之间的协同作用,以促进(3H)-乙酰胆碱从大鼠运动神经末梢释放。

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摘要

The effect of vasoactive intestinal peptide (VIP) on evoked [(3)H]-acetylcholine ([(3)H]-ACh) release from motor nerve terminals, and its interaction with presynaptic facilitatory A(2A)-adenosine receptors was investigated in the rat phrenic nerve-hemidiaphragms. Facilitation of [(3)H]-ACh release by VIP (100 nM) only becomes apparent when high frequency (50 Hz) or long lasting pulses (1 ms) were delivered to the phrenic nerve; VIP excitation was prevented by removal of endogenous adenosine tonus, with adenosine deaminase (2.5 units/ml) or with the A(2A)-receptor antagonist, 3,7-dimethyl-1-propargyl xanthine, (10 microM). Pretreatment with the selective A(2A)-receptor agonist, CGS 21680C (2 nM), potentiated the neurofacilitatory action of VIP (100 nM). The results suggest that tonic A(2A)-receptors activation by endogenous adenosine is required to trigger the facilitatory action of VIP on evoked [(3)H]-ACh release from motor nerve endings.
机译:血管活性肠肽(VIP)对诱发的[(3)H]-乙酰胆碱([(3)H] -ACh)从运动神经末梢的释放及其与突触前促进性A(2A)-腺苷受体相互作用的影响在大鼠神经半ph中。 VIP(100 nM)促进[(3)H] -ACh释放仅在向(神经传递高频(50 Hz)或长脉冲(1 ms)时才明显;通过用腺苷脱氨酶(2.5单位/ ml)或A(2A)受体拮抗剂3,7-二甲基-1-炔丙基黄嘌呤(10 microM)去除内源性腺苷酸来防止VIP兴奋。用选择性A(2A)受体激动剂CGS 21680C(2 nM)预处理可增强VIP(100 nM)的神经促进作用。结果表明,需要由内源性腺苷激活强直性A(2A)受体来触发VIP对诱发​​的[(3)H] -ACh从运动神经末梢释放的促进作用。

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