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胆碱能和组胺能在脑啡肽类似物FK 33 - 824对人体生长激素释放作用中的参与情况。

Cholinergic and histaminergic involvement in the growth hormone releasing effect of an enkephalin analog FK 33-824 in man.

作者信息

Peñalva A, Villanueva L, Casanueva F, Cavagnini F, Gomez-Pan A, Müller E E

出版信息

Psychopharmacology (Berl). 1983;80(2):120-4. doi: 10.1007/BF00427953.

Abstract

Studies were performed in healthy subjects to ascertain the neurotransmitter systems involved in the growth hormone (GH)-releasing effect of the potent enkephalin analog FK 33-824. Concomitant evaluation of prolactin (PRL) secretion was also performed in the same subjects. FK 33-824 at a dose of 0.5 mg IV elicited a clear-cut rise in plasma GH and PRL concentrations with peak levels at 45 min. Blockade of muscarinic cholinergic receptors by atropine (0.5 mg SC) or histaminergic H1 receptors by diphenhydramine (50 mg IV bolus plus 50 mg infusion) completely suppressed the GH release induced by FK 33-824, without significantly altering the PRL rise induced by the peptide. Pretreatment with the alpha-adrenergic antagonist phentolamine (0.5 mg IV/min for 120 min) or the dopamine receptor blocker metoclopramide (10 mg IV) did not alter the GH-releasing effect of FK 33-824. Phentolamine failed to alter the PRL rise induced by FK 33-824, while combined FK 33-824-metoclopramide administration induced a greater PRL increase than FK 33-824 alone. These results indicate that cholinergic and histaminergic H1 receptors play an important role in the GH-release induced by FK 33-824 in man, whereas this action seems to occur independently of catecholaminergic mediation. The same receptors are not involved in the PRL-releasing effect of the peptide.

摘要

在健康受试者中进行了研究,以确定强效脑啡肽类似物FK 33 - 824的生长激素(GH)释放作用所涉及的神经递质系统。同时,对同一受试者的催乳素(PRL)分泌也进行了评估。静脉注射0.5 mg的FK 33 - 824可使血浆GH和PRL浓度明显升高,在45分钟时达到峰值水平。阿托品(0.5 mg皮下注射)阻断毒蕈碱胆碱能受体或苯海拉明(50 mg静脉推注加50 mg输注)阻断组胺能H1受体,可完全抑制FK 33 - 824诱导的GH释放,而不会显著改变该肽诱导的PRL升高。用α - 肾上腺素能拮抗剂酚妥拉明(0.5 mg静脉注射/分钟,共120分钟)或多巴胺受体阻滞剂甲氧氯普胺(10 mg静脉注射)预处理,不会改变FK 33 - 824的GH释放作用。酚妥拉明未能改变FK 33 - 824诱导的PRL升高,而联合使用FK 33 - 824和甲氧氯普胺诱导的PRL升高比单独使用FK 33 - 824更大。这些结果表明,胆碱能和组胺能H1受体在人类FK 33 - 824诱导的GH释放中起重要作用,而这种作用似乎独立于儿茶酚胺能介导发生。相同的受体不参与该肽的PRL释放作用。

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