钠基低渗透压对动脉平滑肌反应性的影响。

M Ezimokhai, N Osman
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引用次数: 3

摘要

该研究验证了正常妊娠的[Na+]e减少和低渗透压与体外血管平滑肌反应性衰减有因果关系的假设。将未怀孕雌性大鼠主动脉环置于114 mM NaCl/l的生理培养基中孵育,比较其对苯肾上腺素、KCl和CaCl2的收缩反应以及对乙酰胆碱和KCl的松弛反应。没有溶质取代降低后的[Na+]。用去内皮环和用吲哚美辛预处理的完整环重复苯肾上腺素实验。低渗透压溶液中完整环(n = 11)对苯肾上腺素的收缩反应显著(P < 0.001)低于正常介质(n = 11)。内皮剥落部分恢复反应,但吲哚美辛不存在。对乙酰胆碱的松弛(n = 7);n = 6(正常溶液)和KCl (n = 7,低渗透压溶液和正常渗透压溶液)在低渗透压溶液中培养的环显著增强(P < 0.05)。在两种溶液中,环对KCl和CaCl2的反应无显著差异。这些影响与之前对正常妊娠血管平滑肌的一些描述相似,表明正常妊娠的[Na+]e减少和低渗透压可能导致血管反应性降低。
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The effect of sodium based hypo-osmolality on arterial smooth muscle reactivity in vitro.

The study tested the hypothesis that the reduced [Na+]e and hypo-osmolality of normal pregnancy are causally linked to the attenuation of vascular smooth muscle reactivity in vitro. Aortic rings from nonpregnant female rats were incubated in physiological medium containing 114 mM NaCl/l and the contractile responses to phenylephrine, KCl and CaCl2 as well as the relaxations to acetylcholine and KCl were compared with those of rings incubated in normal medium containing 119 mM NaCl/l. There was no solute substituted for the lowered [Na+]. Experiments with phenylephrine were repeated using de-endothelialized rings and intact rings pretreated with indomethacin. Contractile responses of intact rings (n = 11) in hypo-osmolar solution to phenylephrine were significantly (P < 0.001) lower than of those in normal medium (n = 11). Responses were partially restored by endothelial denudation but not in the presence of indomethacin. Relaxations to acetylcholine (n = 7 for hypo-osmolar; n = 6 for normal solution) and KCl (n = 7 for each of hypo- and normal osmolar) were significantly enhanced (P < 0.05) in rings incubated in hypo-osmolar solution. There was no significant difference between the responses of the rings to KCl, and CaCl2 in either solution. These effects are similar to some of those previously described for vascular smooth muscle in normal pregnancy suggesting that the reduced [Na+]e and hypo-osmolarity of normal pregnancy may be contributing to the diminished vascular reactivity.

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