正常血压和高血压大鼠心脏发育过程中阿片受体的表达。

Expression of opioid receptors during heart ontogeny in normotensive and hypertensive rats.

作者信息

Zimlichman R, Gefel D, Eliahou H, Matas Z, Rosen B, Gass S, Ela C, Eilam Y, Vogel Z, Barg J

机构信息

Department of Internal Medicine, Hebrew University-Hadassah Medical School, Jerusalem, Israel.

出版信息

Circulation. 1996 Mar 1;93(5):1020-5. doi: 10.1161/01.cir.93.5.1020.

DOI:10.1161/01.cir.93.5.1020

PMID:8598065

Abstract

BACKGROUND

The opioidergic systems are involved in modulating nociceptive stimuli. In addition, the recent results suggest that endogenous and exogenous opioids could play a role in the modulation of blood pressure and cardiac functions. However, little is known regarding the expression and role of opioid-binding sites in the heart. The decreased sensitivity to noxious stimuli in hypertensive rats raises the possibility of different developmental pattern expression of opioid-binding sites in normotensive versus hypertensive rats.

METHODS AND RESULTS

Opioid receptor expression in hearts from hypertensive and normotensive rats was studied during heart development by binding assays. From P1 until P90, the development of the heart in the two rat strains was accompanied by a gradual increase in the density of kappa-opioid receptors. Hearts from hypertensive rats expressed significantly higher levels of kappa receptors compared with those of normotensive rats. At ages older than P7, mu-opioid receptors could not be detected in hearts of both strains, whereas delta-opioid-binding sites gradually increased until reaching adult levels. Seven-day-old cardiomyocyte cultures of both rat strains expressed similar densities of delta or kappa receptors to those observed in hearts from 7-day-old neonates. The mu-binding sites were not detected in cardiomyocytes cultures. Similar to the in vivo state, cultured myocytes from hypertensive rats had significantly higher levels of kappa-binding sites (1.5 fold) compared with those of normotensive rats. The kappa sites are pertussis toxin sensitive, and the state of coupling of the receptor to G protein is similar for the two rat strains.

CONCLUSION

The role of opioid-binding sites in the heart is not completely clear. Hypertensive rats are known to be less sensitive to noxious stimuli compared with normotensive rats. It is controversial whether the site if application of noxious stimuli plays an important role in the sensitivity to pain in hypertensive rats. We suggest that the opioidergic system could play a role in the modulation of blood pressure in addition to its known effect on nociception.

摘要

背景

阿片能系统参与调节伤害性刺激。此外，最近的研究结果表明，内源性和外源性阿片类物质可能在血压和心脏功能的调节中发挥作用。然而，关于阿片结合位点在心脏中的表达和作用，我们所知甚少。高血压大鼠对有害刺激的敏感性降低，这增加了正常血压大鼠与高血压大鼠阿片结合位点不同发育模式表达的可能性。

方法与结果

通过结合试验研究了高血压大鼠和正常血压大鼠心脏在心脏发育过程中的阿片受体表达。从出生后第1天（P1）到第90天（P90），两种大鼠品系心脏的发育伴随着κ-阿片受体密度的逐渐增加。与正常血压大鼠相比，高血压大鼠心脏中κ受体的表达水平显著更高。在P7之后的年龄段，两种品系大鼠的心脏中均未检测到μ-阿片受体，而δ-阿片结合位点逐渐增加直至达到成年水平。两种大鼠品系7天大的心肌细胞培养物中δ或κ受体的密度与7天大的新生大鼠心脏中观察到的相似。在心肌细胞培养物中未检测到μ结合位点。与体内状态相似，与正常血压大鼠相比，高血压大鼠培养的心肌细胞中κ结合位点水平显著更高（1.5倍）。κ位点对百日咳毒素敏感，两种大鼠品系中受体与G蛋白的偶联状态相似。