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ACE2 expression and activity are enhanced during pregnancy

机译:怀孕期间ACE2的表达和活性增强

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ACE2 expression and activity are enhanced during pregnancy. Am J Physiol Regul Integr Comp Physiol 295: R1953-R1961, 2008. First published October 22, 2008; doi:10.1152/ajpregu.90592.2008.-In the current study, we investigated the expression and activity of ACE2 during pregnancy in normotensive and hypertensive rats, focusing on the relative contribution of the uterus and the placentas, the kidney serving as a reference. We used the Sabra rat model of salt-sensitive hypertension. We confirmed a systemic vasodilatory state during the third trimester of pregnancy, as evidenced by a reduction in blood pressure, both in normotensive and hypertensive rats. At the time that blood pressure was reduced, ACE2 was expressed abundantly in the reproductive organs. The relative levels of ACE2 mRNA in the pregnant animal were placenta > kidneys > uterus and of ACE2 activity kidney > placenta > uterus. In the uterus and the placenta, ACE2 expression was unaffected by strain, salt-loading, or the level of blood pressure. ACE2 activity in the uterus of the nonpregnant rat was not affected by any of these variables either, but during pregnancy increased in salt-loaded animals. When estimating the total contribution of the uterus to ACE2 mRNA and activity during pregnancy, we found that the amount of ACE2 mRNA increased in both strains irrespective of diet, but that ACE2 activity increased only in salt-loaded animals. We further estimated the relative total contribution of the uterus, placentas, and kidneys to ACE2 expression and activity during pregnancy by adjusting for mass and number of organs and found that the placentas were the major contributors, followed by the kidney and the uterus. We conclude that during pregnancy, the placentas, in particular, but also the uterus, constitute important sources of ACE2, in addition to its normal production in the kidney, leading to an estimated twofold increase in total ACE2 activity. These data are consistent the hypothesis that transient ACE2 overexpression and increased activity during pregnancy may be important in modulating systemic, as well as local hemodynamics in the uteroplacental unit
机译:怀孕期间ACE2的表达和活性增强。 Am J Physiol Regul Integr Comp Physiol 295:R1953-R1961,2008年。2008年10月22日首次发布。 doi:10.1152 / ajpregu.90592.2008 .--在本研究中,我们研究了正常血压和高血压大鼠怀孕期间ACE2的表达和活性,重点是子宫和胎盘的相对作用,肾脏作为参考。我们使用了盐敏感性高血压的Sabra大鼠模型。我们证实,在妊娠晚期,血压正常和高血压的大鼠均出现了全身性血管舒张状态,这可以通过降低血压来证明。在血压降低时,ACE2在生殖器官中大量表达。怀孕动物中ACE2 mRNA的相对水平为胎盘>肾脏>子宫,ACE2活性的相对水平为肾脏>胎盘>子宫。在子宫和胎盘中,ACE2表达不受应变,盐负荷或血压水平的影响。未怀孕大鼠子宫中的ACE2活性也不受任何这些变量的影响,但在怀孕期间盐负荷动物的ACE2活性增加。在估计子宫对妊娠期间子宫对ACE2 mRNA和活性的总贡献时,我们发现两种品系中的ACE2 mRNA量均增加,而与饮食无关,但是ACE2活性仅在食盐动物中增加。通过调整器官的质量和数量,我们进一步估计了子宫,胎盘和肾脏在妊娠期间对ACE2表达和活性的相对总贡献,并发现胎盘是主要贡献者,其次是肾脏和子宫。我们得出的结论是,在怀孕期间,胎盘,尤其是子宫,还构成子宫内ACE2的重要来源,除了在肾脏中正常产生外,还导致ACE2总活性估计增加了两倍。这些数据符合以下假设:怀孕期间短暂的ACE2过表达和活动增加可能对调节胎盘单位的全身以及局部血流动力学很重要

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