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Pregnancy does not alter the response of uterine arteries to vasoactive intestinal polypeptide.

机译:怀孕不会改变子宫动脉对血管活性肠多肽的反应。

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摘要

In order to provide sufficient nutrients for fetal development, pregnancy is associated with a significant increase in uterine blood flow. Although vasoactive intestinal polypeptide (VIP) is considered to be an important regulator of uterine blood flow it is not known whether endothelium-derived relaxing factors contribute to VIP action in the uterine artery, whether pregnancy alters the effect of VIP in the uterine artery and/or whether VIP interacts with noradrenaline and acetylcholine on the uterine artery and whether pregnancy regulates this possible interaction. In the present study, VIP induced a concentration-dependent relaxation of guinea pig uterine arterial rings, both intact and denuded of endothelium. Pregnancy did not alter the relaxation of uterine artery in response to VIP. In all preparations, addition of N(G)-monomethyl-L-arginine (L-NMMA), indomethacin and diethylcarbamazine did not modify the effect of VIP in uterine arteries. The VIP-receptor complex dissociation constant did not differ significantly between studied vessels, and in all experimental groups the relationship between receptor occupancy and the response was linear, with the receptor reserve (K(A)/EC(50)) close to unity. VIP did not modulate acetylcholine-induced relaxation or noradrenaline-induced contraction in both non-pregnant and pregnant guinea pig uterine arteries. This study has shown that: (i) VIP induces relaxation of guinea pig uterine artery acting as a partial agonist on receptors localized in smooth muscle; (ii) pregnancy does not alter the response of guinea pig uterine arteries to VIP and does not change the receptor affinity for VIP, the efficiency of the receptor coupling or the VIP receptor density; and (iii) VIP does not modulate effects of neurotransmitters on guinea pig uterine arteries and pregnancy is not associated with the changes of VIP-neurotransmitter interaction.
机译:为了为胎儿发育提供足够的营养,妊娠与子宫血流量的显着增加有关。尽管血管活性肠多肽(VIP)被认为是子宫血流的重要调节剂,但尚不清楚内皮源性舒张因子是否对子宫动脉VIP起作用,妊娠是否会改变VIP在子宫动脉中的作用和/ VIP是否会与子宫动脉上的去甲肾上腺素和乙酰胆碱发生相互作用,以及妊娠是否会调节这种可能的相互作用。在本研究中,VIP诱导了豚鼠子宫动脉环的浓度依赖性松弛,无论内皮完整还是裸露。妊娠并没有改变对VIP的子宫动脉松弛。在所有制剂中,添加N(G)-单甲基-L-精氨酸(L-NMMA),消炎痛和二乙基氨基甲嗪都不会改变VIP在子宫动脉中的作用。 VIP-受体复合物的解离常数在所研究的血管之间没有显着差异,并且在所有实验组中,受体占有率与反应之间的关系是线性的,受体储备(K(A)/ EC(50))接近于1。 VIP在未怀孕和怀孕的豚鼠子宫动脉中均未调节乙酰胆碱引起的松弛或去甲肾上腺素引起的收缩。该研究表明:(i)VIP诱导豚鼠子宫动脉舒张,对平滑肌局部受体起部分激动剂的作用; (ii)怀孕不会改变豚鼠子宫动脉对VIP的反应,也不会改变受体对VIP的亲和力,受体偶联的效率或VIP受体密度; (iii)VIP不会调节豚鼠子宫动脉神经递质的作用,并且妊娠与VIP与神经递质相互作用的变化无关。

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