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A new approach regarding the treatment of preeclampsia and preterm labor.

机译:一种治疗先兆子痫和早产的新方法。

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摘要

Both preeclampsia and preterm delivery are important complications in pregnancy and are leading causes for maternal and perinatal morbidity and mortality. The underlying molecular mechanisms of both diseases remain unknown, thus treatments (beta2-stimulants and magnesium sulfate) are essentially symptomatic. Both molecules have molecular weights less than 5-8 kDa and cross the placental barrier thus exerting their effects on the fetus. In addition, the fetus produces peptide hormones that are highly vasoactive and uterotonic and increase in response to maternal stress and with continued development. Fetal peptides are also small molecules that inevitably leak across into the maternal circulation. Aminopeptidases such as placental leucine aminopeptidase (P-LAP) and aminopeptidase A (APA) are large molecules that do not cross the placental barrier. We have shown that APA acts as an antihypertensive agent in the pregnant spontaneously hypertensive rat by degrading vasoactive peptides and as a result returns the animal to a normotensive state. We have also noted that P-LAP acts as an anti-uterotonic agent by degrading uterotonic peptides, and as a result prolongs gestation in the pregnant mouse. Thus, P-LAP and APA represent promising agents for the treatment of preeclampsia and preterm labor by degrading bioactive hormones derived from the feto-placental circulation.
机译:子痫前期和早产都是孕妇的重要并发症,并且是孕产妇和围产儿发病和死亡的主要原因。两种疾病的潜在分子机制仍是未知的,因此治疗(β2-兴奋剂和硫酸镁)本质上是对症治疗。两种分子的分子量均小于5-8 kDa,并穿过胎盘屏障,从而对胎儿产生影响。另外,胎儿产生的肽激素具有高度的血管活性和子宫收缩能力,并随着母体压力的增加和持续发育而增加。胎儿肽也是不可避免地渗漏到母体循环中的小分子。氨基肽酶,例如胎盘亮氨酸氨基肽酶(P-LAP)和氨基肽酶A(APA)是不会穿过胎盘屏障的大分子。我们已经表明,APA通过降解血管活性肽在妊娠自发性高血压大鼠中充当降压药,从而使动物恢复到正常血压状态。我们还注意到,P-LAP通过降解子宫缩蛋白肽而充当抗子宫缩蛋白剂,因此延长了妊娠小鼠的妊娠。因此,P-LAP和APA代表有希望的药物,可通过降解源自胎盘循环的生物活性激素来治疗先兆子痫和早产。

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