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尿精氨酸加压素:新生儿期的排泄模式

Urinary arginine vasopressin: pattern of excretion in the neonatal period.

作者信息

Wiriyathian S, Rosenfeld C R, Arant B S, Porter J C, Faucher D J, Engle W D

出版信息

Pediatr Res. 1986 Feb;20(2):103-8. doi: 10.1203/00006450-198602000-00001.

Abstract

The pattern of arginine vasopressin (AVP) secretion in the immediate neonatal period is unclear. Plasma concentrations of AVP are reflected by its urinary excretion, thus providing a noninvasive method for studying the pattern of AVP release in the neonate. In these studies, we determined the pattern of urinary AVP excretion (microU/mg creatinine) during the first 2-4 days after birth in 78 neonates, 53 of whom had various prenatal and/or neonatal complications. In well term (n = 12) and preterm (n = 13) infants mean urinary AVP excretion decreased gradually during the first 24-36 h after birth. Although term and preterm infants with perinatal asphyxia had highest initial levels of urinary AVP (greater than 200 microU/mg creatinine) and a significant negative correlation with the 1-min Apgar score was obtained, their pattern of excretion was similar to respective controls. After delivery, elevated values for urinary AVP excretion were found among infants with neonatal courses complicated by intracranial hemorrhage, hypoxic encephalopathy, and pneumothorax. Urine osmolality did not correlate linearly with urinary AVP levels, but rather attained a maximum value of approximately 400 mosmol/kg at urinary AVP levels less than 200 microU/mg creatinine and then plateaued. It is concluded that the decrease in urinary AVP excretion observed soon after birth generally reflects diminution of the hypersecretion of AVP during parturition; neonates with evidence of intrapartum asphyxia initially have increased urinary AVP excretion; however, the pattern of excretion is similar to normal infants. During the neonatal period insults such as pneumothorax and intracranial hemorrhage may cause hypersecretion of this hormone.

摘要

新生儿早期精氨酸加压素(AVP)的分泌模式尚不清楚。AVP的血浆浓度可通过其尿排泄量反映出来,从而为研究新生儿AVP释放模式提供了一种非侵入性方法。在这些研究中,我们测定了78例新生儿出生后最初2 - 4天内尿AVP排泄量(微单位/毫克肌酐),其中53例有各种产前和/或新生儿并发症。足月(n = 12)和早产(n = 13)婴儿出生后最初24 - 36小时内尿AVP平均排泄量逐渐下降。尽管围产期窒息的足月和早产婴儿尿AVP初始水平最高(大于200微单位/毫克肌酐),且与1分钟阿氏评分呈显著负相关,但其排泄模式与各自的对照组相似。分娩后,在患有颅内出血、缺氧性脑病和气胸等新生儿疾病的婴儿中发现尿AVP排泄量升高。尿渗透压与尿AVP水平并非呈线性相关,而是在尿AVP水平低于200微单位/毫克肌酐时达到约400毫摩尔/千克的最大值,然后趋于平稳。结论是,出生后不久观察到的尿AVP排泄量下降通常反映了分娩期间AVP分泌过多现象的减少;有产时窒息证据的新生儿最初尿AVP排泄量增加;然而,排泄模式与正常婴儿相似。在新生儿期,气胸和颅内出血等损伤可能导致这种激素分泌过多。

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