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首页> 美国卫生研究院文献>The Journal of Clinical Investigation >In vitro prostacyclin production by ovine uterine and systemic arteries. Effects of angiotensin II.
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In vitro prostacyclin production by ovine uterine and systemic arteries. Effects of angiotensin II.

机译:绵羊子宫和全身动脉的体外前列环素生产。血管紧张素II的作用。

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Normal pregnancy is associated with reduced systemic pressor responses to infused angiotensin II (ANG II); furthermore, the uterine vascular bed is even less responsive to vasoconstriction by ANG II than the systemic vasculature overall. The mechanism(s) for this refractoriness remains unknown. To determine if vessel production of prostacyclin may be responsible, uterine and omental artery segments were obtained from four groups of sheep, nonpregnant (NP), pregnant (P; 131 +/- 4 d), early postpartum (2.2 +/- 0.4 d), and late postpartum (16 +/- 2 d), and incubated in Krebs-Henseleit alone or with ANG II in the absence or presence of Saralasin. Prostacyclin was measured as 6-keto-prostaglandin F1 alpha (6-keto-PGF1 alpha). Synthesis of 6-keto-PGF1 alpha was de novo, since aspirin inhibited its formation. P and early uterine arteries produced more 6-keto-PGF1 alpha than NP and late vessels (P less than 0.05): 386 +/- 60 (X +/- SE) and 175 +/- 23 vs. 32 +/- 5 and 18 +/- 4 pg/mg X h, respectively. A similar relationship was observed for omental arteries: 101 +/- 14 and 74 +/- 14 vs. 36 +/- 10 and 22 +/- 4 pg/mg X h, respectively. Furthermore, synthesis by arteries from P and early animals was greater in uterine than omental vessels (P less than 0.05); this was not observed in NP or late vessels. ANG II increased 6-keto-PGF1 alpha production 107 +/- 20% and 92 +/- 16% in P and early uterine arteries only; the threshold dose was between 5 X 10(-11) and 5 X 10(-9) M ANG II. This ANG II-induced increase in 6-keto-PGF1 alpha by uterine arteries was inhibited by Saralasin, which by itself had no effect. During pregnancy, the reduced systemic pressor response to ANG II and the even greater refractoriness of the uterine vascular bed may be reflective of vessel production of the potent vasodilator, prostacyclin. Furthermore, in the uterine vasculature, this antagonism may be potentiated by specific ANG II receptor-mediated increases in prostacyclin.
机译:正常妊娠与输注血管紧张素II(ANG II)的全身升压反应降低有关;此外,子宫血管床对ANG II血管收缩的反应甚至不及全身血管系统。这种耐火度的机制仍然未知。为了确定是否可能产生前列环素的血管生成,从四组绵羊中获得子宫和网膜动脉段,即非妊娠(NP),孕妇(P; 131 +/- 4 d),产后早期(2.2 +/- 0.4 d) )和产后晚期(16 +/- 2 d),在没有或不存在Saralasin的情况下,在Krebs-Henseleit中单独孵育或与ANG II孵育。前列环素被测量为6-酮-前列腺素F1α(6-酮-PGF1α)。因为阿司匹林抑制了它的形成,所以从头开始合成6-酮-PGF1α。 P和子宫早期动脉比NP和晚期血管产生更多的6-keto-PGF1α(P小于0.05):386 +/- 60(X +/- SE)和175 +/- 23 vs. 32 +/- 5和18 +/- 4 pg / mg X h。对于网膜动脉观察到类似的关系:分别为101 +/- 14和74 +/- 14 vs. 36 +/- 10和22 +/- 4 pg / mg X h。此外,P和早期动物的动脉在子宫中的合成比网膜血管要大(P小于0.05)。在NP或晚期血管中未观察到此现象。 ANG II仅在P和早期子宫动脉中使6-酮-PGF1α产生增加107 +/- 20%和92 +/- 16%。阈剂量在5 X 10(-11)和5 X 10(-9)M ANG II之间。萨拉拉斯(Saralasin)抑制了ANG II引起的子宫动脉6-酮-PGF1α的增加,而它本身没有作用。在怀孕期间,对ANG II的全身性升压反应降低以及子宫血管床的更大耐火度可能反映了有效的血管扩张剂前列环素的血管生成。此外,在子宫脉管系统中,这种拮抗作用可通过前列环素的特定ANG II受体介导的增加而增强。

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