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一种偏好生长抑素的多酪氨酸化sst1/2受体激动剂可抑制豚鼠结肠的反射性和免疫介导性分泌。

A multi-tyrosinated sst1/2 receptor preferring somatostatin agonist inhibits reflex and immune-mediated secretion in the guinea pig colon.

作者信息

Cooke Helen J, Wang Yu-Zhong, Wray Dawn, O'Dorisio M Sue, Woltering Eugene A, Coy David H, Murphy William A, Christofi Fievos L, Gosh Pradip, O'Dorisio Thomas M

机构信息

Department of Neuroscience, The Ohio State University, Columbus, OH 43210, USA.

出版信息

Regul Pept. 2003 Jun 15;114(1):51-60. doi: 10.1016/s0167-0115(03)00108-3.

Abstract

Somatostatin and its analogs such as WOC 3B were compared for their ability to alter the release of 5-hydroxytryptamine (5-HT) and prostaglandins and to affect chloride secretory capacity, determined by activity of neural reflexes or by the influence of immune mediators and other secretagogues. In guinea pig colon set up in flux chambers, the multi-tyrosinated sst1/sst2 receptor preferring somatostatin agonist, WOC 3B, inhibited stroking-evoked 5-HT release without affecting basal release. WOC 3B had no effect on stroking-induced or basal prostaglandin E2 release (PGE2). Neither 5-HT nor PGE2 release was dependent on neural input. Tetrodotoxin induced a decrease in basal short circuit current (Isc) indicative of a decrease in chloride secretion. The decrease in basal Isc during neural blockade was highly correlated with the decrease in basal Isc when WOC 3B was used. In piroxicam- and atropine-treated tissues, to eliminate prostaglandins and cholinergic muscarinic input to crypts, WOC 3B further reduced the piroxicam-resistant and not the atropine resistant Isc during brush stroking the mucosa. Somatostatin and WOC 3B reduced the stroking-evoked Isc with similar half maximum concentrations of 1-2 nM. WOC 3B reduced by more than 50% dimaprit-evoked cyclical Isc. The rank order of potencies in inhibiting dimaprit-evoked Isc was: Somatostatin-14=WOC 3B>CH275=DC-32-92>DC-23-48>> >>DC-32-87=DC-32-97. Low nanomolar concentrations of WOC 3B primarily inhibited the neural effects of carbachol and forskolin on Isc without altering their epithelial effects. Equi-molar concentrations (4 nM) of CH275, a somatostatin sst1 receptor agonist, and the somatostatin sst2 receptor agonist, [Tyr(3)]-octreotide, inhibited dimaprit-evoked Isc by 25% and 26%, and their effects were additive. The results suggest that WOC 3B, a somatostatin analogue containing three tyrosine residues, has anti-secretory effects due to activation of somatostatin sst1 and sst2 receptors on enteric neurons.

摘要

比较了生长抑素及其类似物如WOC 3B改变5-羟色胺(5-HT)和前列腺素释放以及影响氯离子分泌能力的作用,氯离子分泌能力通过神经反射活性或免疫介质及其他促分泌剂的影响来确定。在置于流通室的豚鼠结肠中,多酪氨酸化的、偏好sst1/sst2受体的生长抑素激动剂WOC 3B抑制轻触诱发的5-HT释放,而不影响基础释放。WOC 3B对轻触诱导的或基础的前列腺素E2(PGE2)释放没有影响。5-HT和PGE2的释放均不依赖于神经输入。河豚毒素导致基础短路电流(Isc)降低,表明氯离子分泌减少。神经阻断期间基础Isc的降低与使用WOC 3B时基础Isc的降低高度相关。在吡罗昔康和阿托品处理的组织中,为消除前列腺素和胆碱能毒蕈碱对隐窝的输入,在轻刷黏膜期间,WOC 3B进一步降低了吡罗昔康抗性而非阿托品抗性的Isc。生长抑素和WOC 3B以相似的半数最大浓度1-2 nM降低轻触诱发的Isc。WOC 3B使二甲弗林诱发的周期性Isc降低超过50%。抑制二甲弗林诱发的Isc的效力顺序为:生长抑素-14 = WOC 3B>CH275 = DC-32-92>DC-23-48>>DC-32-87 = DC-32-97。低纳摩尔浓度的WOC 3B主要抑制卡巴胆碱和福斯高林对Isc的神经作用,而不改变它们对上皮的作用。生长抑素sst1受体激动剂CH275和生长抑素sst2受体激动剂[Tyr(3)]-奥曲肽的等摩尔浓度(4 nM)分别使二甲弗林诱发的Isc抑制25%和26%,且它们的作用是相加的。结果表明,含有三个酪氨酸残基的生长抑素类似物WOC 3B由于激活肠神经元上的生长抑素sst1和sst2受体而具有抗分泌作用。

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