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Smooth muscle 5-HT2A receptors mediating contraction of porcine isolated proximal stomach strips

机译:平滑肌5-HT2A受体介导猪离体近端胃条收缩

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摘要

class="enumerated" style="list-style-type:decimal">The aim of this study was to characterize the 5-HT receptors involved in the 5-HT-induced contraction of longitudinal muscle (LM) strips of porcine proximal stomach. This was done in a classical organ bath set-up for isotonic measurement.The concentration-contraction curve to 5-HT was not modified by 5-HT3 and 5-HT4 receptor antagonism. Methysergide, ketanserin and mesulergine antagonized the curve to 5-HT. Concomitantly, increasing concentrations of ketanserin and mesulergine progressively revealed a biphasic nature of the 5-HT curve. Ketanserin antagonized the low-affinity receptor while it did not modify the high-affinity receptor.Tetrodotoxin did not influence the concentration-contraction curve to 5-HT neither in the absence nor presence of ketanserin, indicating that nerves are not involved.Ketanserin competitively antagonized the monophasic concentration-response curve to α-Methyl-5-HT, yielding a Schild slope that was not significantly different from unity. After constraining the Schild slope to unity, a pKB estimate of 8.23±0.90 was obtained. This affinity estimate of ketanserin closely approximates previously reported affinities at 5-HT2A receptors.In the presence of ketanserin (0.1 μM; exposing the high-affinity receptor), a wide range of 5-HT receptor antagonists covering all 5-HT receptors known, was tested. Only methysergide and ritanserin inhibited the response to 5-HT, thus expressing affinity for the high-affinity receptor. This did not reveal the identity of the receptor involved.It can be concluded that 5-HT induces pig proximal stomach (LM) contraction via 5-HT2A receptors located on smooth muscle. A ketanserin-insensitive phase of contractions could not be characterized between the actually known classes of 5-HT receptors with the pharmacological tools that were used.
机译:class =“ enumerated” style =“ list-style-type:decimal”> <!-list-behavior =枚举前缀-word = mark-type = decimal max-label-size = 0-> 这项研究的目的是表征5-HT受体参与猪近端胃纵肌(LM)条的5-HT诱导的收缩。这是在用于等渗测量的经典器官浴装置中完成的。 5-HT3和5-HT4受体拮抗作用不会改变5-HT的浓度-收缩曲线。 Methysergide,ketanserin和mesulergine将曲线拮抗为5-HT。随之而来的是,增加的酮色林和美司麦碱浓度逐渐显示出5-HT曲线的两相性质。 Ketanserin拮抗低亲和力受体,而不会修饰高亲和力受体。 河豚毒素在不存在或不存在酮色林的情况下均不影响5-HT的浓度-收缩曲线,表明神经 Ketanserin竞争性地拮抗α-Methyl-5-HT的单相浓度-响应曲线,产生的Schild斜率与统一无明显差异。将Schild斜率约束为1之后,pKB估计为8.23±0.90。酮色林的亲和力估计值与先前报道的对5-HT2A受体的亲和力非常接近。 在存在酮色林(0.1μM;暴露高亲和力受体)的情况下,广泛的5-HT受体拮抗剂测试了所有已知的5-HT受体。仅美塞麦肽和利坦色林抑制了对5-HT的应答,因此表达了对高亲和力受体的亲和力。这并未揭示所涉及受体的身份。 可以得出结论,5-HT通过位于平滑肌上的5-HT2A受体诱导猪近端胃(LM)收缩。酮色林不敏感的收缩期无法通过所使用的药理学工具在实际已知的5-HT受体之间进行表征。

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