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Nitric oxide metabolism in the human placenta during aberrant maternal inflammation

机译:在异常母体炎症期间人胎盘中的一氧化氮代谢

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Key points Nitric oxide (NO) is a gasotransmitter with important physiological and pathophysiological roles in pregnancy. There is limited information available about the sources and metabolism of NO and its bioactive metabolites (NOx) in both normal and complicated pregnancies. The present study characterized and quantified endogenous NOx in human and mouse placenta following determination of the stability of exogenous NOx in placental homogenates. NOx have differential stability in placental homogenates. NO and iron nitrosyl species (FeNOs), are relatively unstable in placental homogenates from normal placentas. Exogenous NO, nitrite and nitrosothiols react with placental homogenates to form iron nitrosyl complexes. FeNOs were also detected endogenously in mouse and human placenta. NOx levels in placental villous tissue are increased in fetal growth restriction vs . placentas from women with normal pregnancies, particularly in fetal growth restriction associated with pre‐eclampsia. Villitis was not associated, however, with an increase in NOx levels in either normotensive or pre‐eclamptic placentas. The results call for further investigation of FeNOs in normal and complicated pregnancies. Abstract Nitric oxide (NO) is a gasotransmitter with important roles in pregnancy under both physiological and pathophysiological conditions. Although products of NO metabolism (NOx) also have significant bioactivity, little is known about the role of NO and NOx under conditions of aberrant placental inflammation during pregnancy. An ozone‐based chemiluminescence approach was used to investigate the stability and metabolic fate of NOx in human placental homogenates from uncomplicated pregnancies in healthy mothers compared to that in placental tissue from normotensive and pre‐eclamptic pregnancies complicated with fetal growth restriction (FGR) with and without villitis of unknown aetiology. We hypothesized that placental NOx would be increased in FGR vs . normal tissue, and be further increased in villitis vs . non‐villitis placentas. Findings indicate that nitrate, nitrite and nitrosothiols, but not NO or iron nitrosyl species (FeNOs), are relatively stable in placental homogenates from normal placentas, and that NO, nitrite and nitrosothiols react with placental homogenates to form iron nitrosyl complexes. Furthermore, NOx levels in placental villous tissue are increased in FGR vs . placentas from women with normal pregnancies, particularly in FGR associated with pre‐eclampsia. However, in contrast to our hypothesis, villitis was not associated with an increase in NOx levels in either normotensive or pre‐eclamptic placentas. Our results also strongly support the involvement of FeNOs in both mouse and human placenta, and call for their further study as a critical mechanistic link between pre‐eclampsia and fetal growth restriction.
机译:关键点一氧化氮(NO)是具有重要的生理和在妊娠病理生理作用一个gasotransmitter。有可用的关于NO和其生物活性的代谢物(NOx)的在正常和复杂怀孕的来源和代谢的有限信息。本研究中,其特征在于与在人类和小鼠胎盘定量内源性的NOx以下判定外源NOx的胎盘匀浆稳定性。的NOx在胎盘匀浆差的稳定性。 NO和亚硝酰基铁物种(FeNOs),都是在从正常胎盘的胎盘匀浆相对不稳定。外源性NO,亚硝酸盐和亚硝基硫醇与胎盘匀浆以形成亚硝酰基铁配合物反应。 FeNOs也分别在小鼠和人类胎盘内源性检测。在胎盘绒毛组织的NOx水平在胎儿生长受限VS增加。从妇女正常妊娠,特别是在胎儿生长受限先兆子痫胎盘相关联。 Villitis不相关联,但是,与在任一血压正常或先兆子痫胎盘的增加的NOx水平。结果要求在正常和怀孕并发症FeNOs的进一步调查。抽象一氧化氮(NO)是具有生理和病理生理条件下,在妊娠重要作用一个gasotransmitter。虽然没有代谢(氮氧化物)的产品也有显著的生物活性,鲜为人知的是,NO和NOx的异常胎盘炎症条件下,妊娠期间的作用。使用基于臭氧的化学发光的方法来调查的NOx在从健康母亲不复杂的妊娠的人胎盘组织匀浆与稳定性和代谢命运相比,在从血压正常和先兆子痫孕妇的胎盘组织与胎儿生长受限(FGR)复杂且无病因不明的villitis。我们假设胎盘氮氧化物会在FGR VS增加。正常组织,并且在villitis VS被进一步增加。非villitis胎盘。研究结果表明,硝酸盐,亚硝酸盐和亚硝基硫醇,但不是NO或亚硝酰基铁物种(FeNOs),是相对稳定的胎盘匀浆从正常胎盘,而NO,亚硝酸盐和亚硝基硫醇与胎盘匀浆以形成亚硝酰基铁配合物反应。此外,在胎盘绒毛组织的NOx水平在FGR VS增加。从女性正常妊娠,尤其是在FGR先兆子痫相关胎盘。然而,与我们的假设,villitis没有用在任何血压正常或先兆子痫胎盘增加NOx水平有关。我们的研究结果也强烈支持FeNOs在小鼠和人胎盘的参与,并呼吁他们进一步研究先兆子痫和胎儿生长受限之间的重要关联机制。

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