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前列腺素在心脏中的合成与功能。

The synthesis and function of prostaglandins in the heart.

作者信息

Needleman P

出版信息

Fed Proc. 1976 Oct;35(12):2376-81.

PMID:786741
Abstract

The isolated perfused rabbit heart has the capacity to rapidly synthesize, release, and inactivate prostaglandins (PGs) which can readily modulate coronary resistance and cardiac performance. Prostaglandin synthetase converts arachidonic acid to prostaglandin-like substance in one passage across the heart. There is little evidence of functional prostaglandin dehydrogenase activity. Arachidonic acid and bradykinin produce a concentration-dependent decrease in coronary resistance directly associated with PG-like substance biosynthesis and release. An inhibitor of bradykinin destruction, the nonapeptide SQ-20881, markedly enhanced both the coronary vasodilation and PG-like substance release produced by cardiac injection of bradykinin. Indomethacin inhibited both the myocardial prostaglandin biosynthesis and the decrease in coronary resistance induced by bradykinin and arachidonic acid. In addition to direct effects on coronary vascular smooth muscle, prostaglandins produced in the heart apparently exert a modulating influence on efferent autonomic and on afferent cardiovascular and pain reflexes.

摘要

离体灌注兔心脏能够快速合成、释放并使前列腺素(PGs)失活,而前列腺素可轻易调节冠状动脉阻力和心脏功能。前列腺素合成酶在一次流经心脏的过程中将花生四烯酸转化为前列腺素样物质。几乎没有证据表明存在功能性前列腺素脱氢酶活性。花生四烯酸和缓激肽会使冠状动脉阻力呈浓度依赖性降低,这与前列腺素样物质的生物合成和释放直接相关。缓激肽破坏抑制剂九肽SQ - 20881显著增强了心脏注射缓激肽所产生的冠状动脉舒张和前列腺素样物质释放。吲哚美辛抑制心肌前列腺素的生物合成以及缓激肽和花生四烯酸诱导的冠状动脉阻力降低。除了对冠状动脉血管平滑肌有直接作用外,心脏产生的前列腺素显然还对传出自主神经以及传入心血管和疼痛反射发挥调节作用。

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