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前列腺素内过氧化物和一种内过氧化物类似物的支气管及心血管作用。

Bronchial and cardiovascular actions of prostaglandin endoperoxides and an endoperoxide analogue.

作者信息

Hedqvist P, Strandberg K, Hamberg M

出版信息

Acta Physiol Scand. 1978 Jul;103(3):299-307. doi: 10.1111/j.1748-1716.1978.tb06217.x.

Abstract

Effects of PGG2, PGH2 and the endoperoxide analogue, EPA, on bronchial and vascular smooth muscle were studied in vivo and in vitro. In the cat PGG2, PGH2 and particularly EPA proved potent stimulators of airway resistance, and they were all significantly more active than PGF2 alpha. They also increased pulmonary vascular resistance but EPA alone was more active than PGF2 alpha. In guinea pigs EPA was 90--190 times more active than PGF2 alpha in increasing tracheal insufflation pressure. Human bronchi contracted in response to PGG2, PGH2 and EPA. PGG2 and PGH2 were equiactive with PGF2 alpha and EPA was more than 500 times as potent. PGG2 and PGH2 lowered systemic arterial blood pressure and increased heart rate in cats. They were as active or more active than PGE2, EPA, on the other hand, resembled PGF2 alpha in producing biphasic changes of blood pressure and heart rate or decrease of blood pressure and bradycardia in guinea pig and cat. The results obtained in this study indicate that PGG2, PGH2 and EPA are potent stimulators of bronchial and pulmonary vascular smooth muscle. The data are also consistent with the view that a significant proportion of effects resulting from prostaglandin generation in the lung is due to prostaglandin endoperoxides rather than primary prostaglandins.

摘要

在体内和体外研究了前列腺素G2(PGG2)、前列腺素H2(PGH2)和内过氧化物类似物依前列醇(EPA)对支气管和血管平滑肌的作用。在猫身上,PGG2、PGH2,尤其是EPA被证明是气道阻力的强效刺激剂,并且它们都比前列腺素F2α(PGF2α)更具活性。它们还增加了肺血管阻力,但仅EPA比PGF2α更具活性。在豚鼠中,EPA在增加气管吹入压力方面的活性比PGF2α高90至190倍。人支气管对PGG2、PGH2和EPA有收缩反应。PGG2和PGH2与PGF2α活性相当,而EPA的效力是PGF2α的500倍以上。PGG2和PGH2可降低猫的体循环动脉血压并增加心率。它们与前列腺素E2(PGE2)活性相当或更高,另一方面,EPA在豚鼠和猫身上产生血压和心率的双相变化或血压降低和心动过缓,这与PGF2α相似。本研究获得的结果表明,PGG2、PGH2和EPA是支气管和肺血管平滑肌的强效刺激剂。这些数据也与以下观点一致,即肺中前列腺素生成所产生的大部分效应是由于前列腺素内过氧化物而非初级前列腺素。

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