Presence of the mu(3) opiate receptor in endothelial cells - Coupling to nitric oxide production and vasodilation

被引:273
|
作者
Stefano, GB
Hartman, A
Bilfinger, TV
Magazine, HI
Liu, Y
Casares, F
Goligorsky, MS
机构
[1] SUNY COLL OLD WESTBURY,NEUROSCI RES INST,OLD WESTBURY,NY 11568
[2] CUNY QUEENS COLL,DEPT BIOL,FLUSHING,NY 11367
[3] CUNY,GRAD SCH,FLUSHING,NY 11367
[4] SUNY STONY BROOK,MED CTR,DIV NEPHROL & HYPERTENS,STONY BROOK,NY 11794
关键词
D O I
10.1074/jbc.270.51.30290
中图分类号
Q5 [生物化学]; Q7 [分子生物学];
学科分类号
071010 ; 081704 ;
摘要
Initial confinement of opiate receptors to the nervous system has recently been broadened to several other cell types. Based on the well established hypotensive effect of morphine, we hypothesized that endothelial cells may represent a target for this opiate substance. Endothelial cells (human arterial and rat microvascular) contain a high affinity, saturable opiate binding site presumed to mediate the morphine effects that is stereoselectively and characteristically antagonized by naloxone. This opiate alkaloid-specific binding site is insensitive to opioid peptides. It is, therefore, considered to be the same subtype of opiate receptor (designated mu(3)) used in the mediation of morphine in other cell types exhibiting the same binding profile. Experiments with endothelial cultures and the aortic ring of rats cultured in vitro demonstrate that morphine exerts direct modulatory control over the activities of endothelial cells, which leads to vasodilation. It induces the production of nitric oxide, a process that is sensitive to naloxone antagonism and nitric oxide synthase inhibition. In contrast with that of opiates, the administration of opioid peptides does not induce nitric oxide production by endothelial cells. In conclusion, the data presented above reveal a novel site of morphine action, endothelial cells, where a mu(3) receptor is coupled to nitric oxide release and vasodilation.
引用
收藏
页码:30290 / 30293
页数:4
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