阿片受体亚型在阿片肽对孕期催乳素分泌的刺激和抑制作用中的参与情况。

Involvement of opioid receptor subtypes in both stimulatory and inhibitory effects of the opioid peptides on prolactin secretion during pregnancy.

作者信息

Soaje M, Deis R P

机构信息

Laboratorio de Reproducción y Lactancia, IMBECUCONICET, Mendoza, Argentina.

出版信息

Cell Mol Neurobiol. 2004 Apr;24(2):193-204. doi: 10.1023/b:cemn.0000018616.00018.98.

DOI:10.1023/b:cemn.0000018616.00018.98

PMID:15176435

原文链接:https://pmc.ncbi.nlm.nih.gov/articles/PMC11529975/

Abstract

We have previously demonstrated the existence of a dual neuromodulatory regulation of prolactin secretion by the opioid system. In the present work, we evaluated the opioid receptor subtypes involved in both the stimulatory and the inhibitory regulation of prolactin secretion in pregnant rats. 2. Specific opioid agonists and antagonists were administered intracerebro ventricular (i.c.v.) to rats on day 3 and on day 19 pregnancy in rats of pretreated with mifepristone. Blood samples were obtained after decapitation at 12.00 and 18.00 h. Serum prolactin levels were measured by RIA. 3. The mu-selective agonist DAMGO and beta-endorphin caused a significant increase in serum prolactin secretion on day 3 of pregnancy, during the diurnal surge and intersurge period. Pretreatment with naloxone prevented the increase on prolactin levels induced by DAMGO. The administration of U-50,488, a kappa-selective agonist or DPDPE, a delta-selective agonist, did not modify serum prolactin concentration while the mu1-antagonist naloxonazine reduced significantly serum prolactin levels. On day 19 of pregnancy, the release of prolactin induced by mifepristone was significantly increase by naloxonazine, while the kappa-antagonist nor-binaltorfimine induced only a small but significant increase. No effect was observed after administration of the delta-antagonist naltrindole. 4. We conclude that the mu-opioid receptor seems to be more specifically involved in both the stimulatory and inhibitory regulation by the opioid system on prolactin secretion during pregnancy. The increase on serum prolactin levels on day 3 after administration of DAMGO and beta-endorphin may suggest the participation of other regulatory mechanisms as the dopaminergic and serotoninergic systems. On day 19, only the endogenous ligands delta did not participate in the regulation of prolactin secretion, while the participation of the kappa-opioid receptor was significantly less effective than the endogenous ligand mu. Our results provide evidences of an important role of the opioid system through specific receptors on the regulation of prolactin secretion during early and late pregnancy.

摘要

我们之前已经证明了阿片系统对催乳素分泌存在双重神经调节作用。在本研究中，我们评估了参与妊娠大鼠催乳素分泌刺激和抑制调节的阿片受体亚型。2. 对米非司酮预处理的妊娠第3天和第19天的大鼠进行脑室内（i.c.v.）注射特定的阿片激动剂和拮抗剂。在12:00和18:00断头后采集血样。通过放射免疫分析（RIA）测定血清催乳素水平。3. μ选择性激动剂DAMGO和β-内啡肽在妊娠第3天的日间高峰和高峰间期导致血清催乳素分泌显著增加。纳洛酮预处理可阻止DAMGO诱导的催乳素水平升高。κ选择性激动剂U-50,488或δ选择性激动剂DPDPE的给药未改变血清催乳素浓度，而μ1拮抗剂纳洛嗪显著降低血清催乳素水平。在妊娠第19天，纳洛嗪显著增加了米非司酮诱导的催乳素释放，而κ拮抗剂去甲二氢吗啡酮仅诱导了小幅度但显著的增加。给予δ拮抗剂纳曲吲哚后未观察到效果。4. 我们得出结论，μ阿片受体似乎更具体地参与了阿片系统在妊娠期间对催乳素分泌的刺激和抑制调节。给予DAMGO和β-内啡肽后第3天血清催乳素水平的升高可能提示多巴胺能和5-羟色胺能系统等其他调节机制的参与。在第19天，只有内源性配体δ不参与催乳素分泌的调节，而κ阿片受体的参与比内源性配体μ的效果显著要低。我们的结果提供了证据，表明阿片系统通过特定受体在妊娠早期和晚期对催乳素分泌的调节中起重要作用。